Clinical Focus


  • Lymphatic Diseases
  • Cardiology (Heart)
  • Cardiology (Heart), Preventive
  • Cardiovascular Disease

Academic Appointments


Administrative Appointments


  • Member, Trans-NIH Angiogenesis Research Program (TARP), National Institutes of Health (2004 - Present)
  • Member, Trans-NIH Coordinating Committee for Lymphatic Research (2002 - Present)
  • Chair, Gordon Research Conference: Molecular Mechanisms of Lymphatic Function and Disease (2002 - 2004)
  • Associate Program Director, Internal Medicine Residency Program, Stanford University (1999 - 2008)
  • Editorial Board, Angiology (1997 - Present)
  • Editor-in-Chief, Lymphatic Research and Biology (2002 - Present)
  • Chair, Scientific Advisory Committee, Lymphatic Research Foundation (1999 - Present)
  • Director, Stanford Center for Lymphatic and Venous Disorders, Stanford University (2000 - Present)
  • Chief of Consultative Cardiology, Stanford University (1997 - Present)
  • Allan and Tina Neill Professor of Lymphatic Research and Medicine, Stanford University (2008 - Present)

Honors & Awards


  • Dean’s Award for Excellence in Teaching, Stanford University (2004)
  • Lymphatic Research Leadership Award, Lymphatic Research Foundation (2004, 2006)
  • Chief Resident’s Teaching Award, Stanford University (2003)
  • Teaching Award in Cardiology, Stanford University (2000)
  • David W. Rytand Award for Excellence in Clinical Teaching, Stanford University (1999)
  • Samuel Levine Fellow, American Heart Association (1977)
  • Roche Award for Clinical Excellence, Duke University (1975)
  • John A. White Fellow, North Carolina Arthritis Foundation (1974-5)
  • Alpha Omega Alpha, Duke University (1973)
  • Phi Beta Kappa, Duke University (1971)
  • David W. Rytand Award for Excellence in Clinical Teaching, Department of Medicine, Stanford University (1999)
  • Teaching Award in Cardiology, Department of Medicine, Stanford University (2000)
  • Chief Residents' Teaching Award, Department of Medicine, Stanford University (2003)
  • Franklin G. Ebaugh Jr. Award for Mentoring Medical Students, Stanford University (2008)
  • E. William Hancock Cardiovascular Medicine Teaching Award, Stanford University (2008)
  • Pioneer Award, Lymphatic Research Foundation (2009)

Boards, Advisory Committees, Professional Organizations


  • Editor-in-Chief, Lymphatic Research and Biology (2002 - Present)
  • Founding Chair, Lymphatic Education and Research Network (LE&RN) (1999 - Present)
  • Board of Directors, American Board of Venous and Lymphatic Medicine (2017 - Present)

Professional Education


  • Fellowship: Massachusetts General Hospital Cardiology Fellowship (1981) MA
  • Residency: Brigham and Women's Hospital Internal Medicine Residency (1977) MA
  • Medical Education: Duke University School of Medicine (1975) NC
  • Board Certification: American Board of Internal Medicine, Cardiovascular Disease (1981)
  • Board Certification: American Board of Internal Medicine, Internal Medicine (1978)

Community and International Work


  • Co-Founder

    Topic

    lymphatic disease

    Partnering Organization(s)

    Lymphatic Education and Research Network (LE&RN)

    Location

    International

    Ongoing Project

    Yes

    Opportunities for Student Involvement

    No

Patents


  • Stanley G. Rockson, Mark R. Nicolls, Wen A. Tian, Xinguo Jiang, Jeanna Kim. "United States Patent 10,500,178 B2 LTB4 Inhibition to Prevent and Treat Human Lymphedema", Leland Stanford Junior University, Oct 10, 2019
  • Raymond Tabibiazar, Stanley G. Rockson. "United States Patent 8,965,708 B2 Method for the Treatment of Acquired Lymphedema", Leland Stanford Junior University, Feb 24, 2015

Current Research and Scholarly Interests


Biomarker identification in lymphatic vascular disease

Drug therapy to reverse lymphatic disease - animal model and pilot human studies

Lymphangiogenesis in Acute and Chronic Experimental Lymphedema

Lymphangiogenesis in Lymphatic Insufficiency: Lymphatic Endothelial and Inflammatory RNA Expression Patterns

Genome-wide Transcriptional Profiling for the Study of Lymphedema Pathobiology,Cellular Signaling Mechanisms and Mechanisms of Therapeutic Lymphangiogenesis

Peripheral Arterial Disease and Critical Limb Ischemia

Randomized trials for the intracoronary infusion of VEGF (vascular endothelial growth factor) to treat advanced coronary artery disease.

Lipid-lowering outcomes trials in coronary and peripheral atherosclerosis.

Clinical outcomes trials to assess therapeutic interventions in post-mastectomy and other forms of lymphedema.

Clinical Trials


  • International Lymphatic Disease and Lymphedema Registry Recruiting

    The purpose of the International Lymphatic Disease and Lymphedema Patient Registry and Biorepository is to collect health information in order to study the disease classification, natural history, and impact of Lymphatic Disease, Lymphedema and Related Disorders and its treatments and medical outcomes.

    View full details

  • Trial of Acebilustat for the Treatment of Upper Arm Lymphedema Recruiting

    This study is designed to investigate the response of unilateral upper extremity (arm) lymphedema, during pharmacologic treatment of lymphedema with oral placebo and oral acebilustat. Participants will receive "study drug" (Acebilustat or placebo), for 9 months. For 3 of these months, the participant will receive placebo; for 6 of these months, the participant will receive active ingredient, acebilustat. The study is blinded which means that the participant will not be told which study pill they are taking.

    View full details

  • Biomarkers for the Detection of Lymphatic Insufficiency Not Recruiting

    Acquired lymphedema is a disease that causes chronic swelling of the limb(s). It is frequently under-recognized or misdiagnosed. This study is designed to lead to the development of an accurate, noninvasive, blood test to allow testing for lymphedema. This approach is particularly useful to investigate relative responses to treatment interventions.

    Stanford is currently not accepting patients for this trial.

    View full details

  • Breast Cancer Lymphedema: Role of Insulin Resistance/FOXC2 Not Recruiting

    To better understand the mechanisms leading to lymphedema development in breast cancer survivors, and the implications for potential innovative approaches to the screening, prevention and treatment of this condition.

    Stanford is currently not accepting patients for this trial. For more information, please contact Anne Marie Vaillant-Newman, (650) 498 - 4460.

    View full details

  • Characterization of Treatment Responses in Lymphedema Not Recruiting

    This study is designed to investigate the treatment response of lymphedema, of the upper or lower extremity, during clinical, pharmacologic treatment of lymphedema with oral ketoprofen. Correlation of clinical responses (changes in limb volume and skin thickness) with changes in the inflammasome will help to define the molecular substrate of treatment response.

    Stanford is currently not accepting patients for this trial. For more information, please contact Leslie Roche, RN, 650-723-1396.

    View full details

  • Lymphedema Prophylaxis in Breast Cancer Survivors Who Show Early Evidence of High-risk Status Not Recruiting

    To compare the effectiveness of usual treatments for lymphedema \[massage and elastic compression sleeve, instituted at-risk and before the development of swelling (lymphedema)\], compared to the use of a newly-marketed device, the Flexitouch, which electronically simulates the effect of massage upon lymph flow.

    Stanford is currently not accepting patients for this trial. For more information, please contact Les Roche, RN, 650-724-5913.

    View full details

  • Lymphedema Study for Arm or Leg Lymphedema Not Recruiting

    This study compares the effectiveness of a study drug versus placebo in the treatment of lymphedema.

    Stanford is currently not accepting patients for this trial. For more information, please contact Leslie Roche, RN, 650-723-1396.

    View full details

  • National Breast Cancer and Lymphedema Registry Not Recruiting

    The purpose of the National Breast Cancer Lymphedema Registry is to collect health information in order to study the lymphedema as a complication of breast cancer treatment. The investigators hope to learn whether early diagnosis will help to prevent lymphedema or, if it does occur, to reduce the severity.

    Stanford is currently not accepting patients for this trial. For more information, please contact Leslie Roche, 650-723-1396.

    View full details

  • Placebo-Controlled Therapeutic Trial for the Prevention of Lymphedema Not Recruiting

    This randomized clinical trial studies an investigational drug in preventing lymphedema in patients at high risk after undergoing axillary lymph node dissection. The study drug may prevent lymphedema in patients undergoing axillary lymph node dissection.

    Stanford is currently not accepting patients for this trial.

    View full details

  • Prospective Evaluation of a Surgical Solution for Breast Cancer-Associated Lymphedema Not Recruiting

    To investigate whether addition of the Biobridge scaffold to the standard surgery for vascularized lymph node transfer will improve the outcome of surgical treatment in lymphedema of the upper arm.

    Stanford is currently not accepting patients for this trial. For more information, please contact Leslie Roche, RN, 650-723-1396.

    View full details

  • Recombinant Human Hyaluronidase in Treating Lymphedema in Patients With Cancer Not Recruiting

    This phase 1-2 trial studies the side effects and the best dose of recombinant human hyaluronidase and to see how well it works in treating lymphedema in patients with cancer. Recombinant human hyaluronidase (r-hu-hyaluronidase, rHuPH20) may reduce limb edema size in patients with lymphedema.

    Stanford is currently not accepting patients for this trial. For more information, please contact Les Roche, 650-723-1396.

    View full details

  • The GORE Viabahn Endoprosthesis for the Treatment of Venous Occlusions and Stenoses Not Recruiting

    To study the safety and efficacy of drug coated stents for the treatment of venous occlusions and stenoses in the lower extremity. The use of the device for the treatment of peripheral arterial disease is approved by the FDA, however, the use of the device in venous occlusions and stenoses, although performed by some practitioners, has not yet been studied in detail.

    Stanford is currently not accepting patients for this trial. For more information, please contact Kamil Unver, 650-725-9810.

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  • Ubenimex in Adult Patients With Lymphedema of The Lower Limb (ULTRA) Not Recruiting

    This proof-of-concept study is designed as a randomized, double-blind, placebo-controlled study comparing ubenimex at 150 mg, 3 times daily (total daily dose of 450 mg) with placebo for 6 months treatment period in patients with leg lymphedema.

    Stanford is currently not accepting patients for this trial. For more information, please contact Eric Henderson, 650-723-1396.

    View full details

2024-25 Courses


All Publications


  • The lymphedema patient experience within the healthcare system: a cross-sectional epidemiologic assessment. Scientific reports Bowman, C., Rockson, S. G. 2024; 14 (1): 12600

    Abstract

    Lymphedema is a progressive lymphatic disease that potentiates physical and psychosocial distress. Despite its impact, patients reportedly encounter lymphatic ignorance throughout the healthcare system. This cross-sectional study aims to summarize clinical characteristics and interactions of lymphedema patients within the healthcare system. Two lymphedema patient cohorts were included: The Global Registry Analysis Cohort included lymphedema patients who contributed to an international digital lymphatic registry and the Interactions Cohort included patients who initiated a questionnaire about interactions with the medical system. The global registry was used to obtain demographic and clinical characteristics from affiliated lymphedema patients. A 23-item online questionnaire on healthcare experiences and satisfaction with lymphatic healthcare was then distributed to the Interactions Cohort. Complete responses were obtained from 2474 participants. Participants were a mean age of 57.5 ± 16.1 years and 51.4% had a cancer history. Participants reported substantial delays in diagnosis and treatment. Cancer-related and non-cancer-related lymphedema patients reported similar levels of perceived physician disinterest in their lymphedema; however, non-cancer-related lymphedema patients reported more care dissatisfaction. Ultimately, patients continue to face delays in lymphedema diagnosis and treatment. We developed an evidence-based model highlighting areas of reform needed to improve lymphatic education and healthcare.

    View details for DOI 10.1038/s41598-024-63145-1

    View details for PubMedID 38824156

    View details for PubMedCentralID 7445072

  • Abnormal Lymphatic Sphingosine-1-Phosphate Signaling Aggravates Lymphatic Dysfunction and Tissue Inflammation. Circulation Kim, D., Tian, W., Wu, T. T., Xiang, M., Vinh, R., Chang, J. L., Gu, S., Lee, S., Zhu, Y., Guan, T., Schneider, E. C., Bao, E., Dixon, J. B., Kao, P., Pan, J., Rockson, S. G., Jiang, X., Nicolls, M. R. 2023

    Abstract

    Lymphedema is a global health problem with no effective drug treatment. Enhanced T-cell immunity and abnormal lymphatic endothelial cell (LEC) signaling are promising therapeutic targets for this condition. Sphingosine-1-phosphate (S1P) mediates a key signaling pathway required for normal LEC function, and altered S1P signaling in LECs could lead to lymphatic disease and pathogenic T-cell activation. Characterizing this biology is relevant for developing much needed therapies.Human and mouse lymphedema was studied. Lymphedema was induced in mice by surgically ligating the tail lymphatics. Lymphedematous dermal tissue was assessed for S1P signaling. To verify the role of altered S1P signaling effects in lymphatic cells, LEC-specific S1pr1-deficient (S1pr1LECKO) mice were generated. Disease progression was quantified by tail-volumetric and -histopathologic measurements over time. LECs from mice and humans, with S1P signaling inhibition, were then cocultured with CD4 T cells, followed by an analysis of CD4 T-cell activation and pathway signaling. Last, animals were treated with a monoclonal antibody specific to P-selectin to assess its efficacy in reducing lymphedema and T-cell activation.Human and experimental lymphedema tissues exhibited decreased LEC S1P signaling through S1P receptor 1 (S1PR1). LEC S1pr1 loss-of-function exacerbated lymphatic vascular insufficiency, tail swelling, and increased CD4 T-cell infiltration in mouse lymphedema. LECs, isolated from S1pr1LECKO mice and cocultured with CD4 T cells, resulted in augmented lymphocyte differentiation. Inhibiting S1PR1 signaling in human dermal LECs promoted T-helper type 1 and 2 (Th1 and Th2) cell differentiation through direct cell contact with lymphocytes. Human dermal LECs with dampened S1P signaling exhibited enhanced P-selectin, an important cell adhesion molecule expressed on activated vascular cells. In vitro, P-selectin blockade reduced the activation and differentiation of Th cells cocultured with shS1PR1-treated human dermal LECs. P-selectin-directed antibody treatment improved tail swelling and reduced Th1/Th2 immune responses in mouse lymphedema.This study suggests that reduction of the LEC S1P signaling aggravates lymphedema by enhancing LEC adhesion and amplifying pathogenic CD4 T-cell responses. P-selectin inhibitors are suggested as a possible treatment for this pervasive condition.

    View details for DOI 10.1161/CIRCULATIONAHA.123.064181

    View details for PubMedID 37609838

  • Human collecting lymphatic glycocalyx identification by electron microscopy and immunohistochemistry. Scientific reports Gianesini, S., Rimondi, E., Raffetto, J. D., Melloni, E., Pellati, A., Menegatti, E., Avruscio, G. P., Bassetto, F., Costa, A. L., Rockson, S. 2023; 13 (1): 3022

    Abstract

    Blood flow is translated into biochemical inflammatory or anti-inflammatory signals based onshear stress type, by means of sensitive endothelial receptors. Recognition of the phenomenon is of paramount importance for enhanced insights into the pathophysiological processes of vascular remodeling. The endothelial glycocalyx is a pericellular matrix, identified in both arteries and veins, acting collectively as a sensor responsive to blood flow changes. Venous and lymphatic physiology is interconnected; however, to our knowledge, a lymphatic glycocalyx structure has never been identified in humans. The objective of this investigation is to identify glycocalyx structures from ex vivo lymphatic human samples. Lower limb vein and lymphatic vessels were harvested. The samples were analyzed by transmission electron microscopy. The specimens were also examined by immunohistochemistry. Transmission electron microscopy identified a glycocalyx structure in human venous and lymphatic samples. Immunohistochemistry for podoplanin, glypican-1, mucin-2, agrin and brevican characterized lymphatic and venous glycocalyx-like structures. To our knowledge, the present work reports the first identification of a glycocalyx-like structure in human lymphatic tissue. The vasculoprotective action of the glycocalyx could become an investigational target in the lymphatic system as well, with clinical implications for the many patients affected by lymphatic disorders.

    View details for DOI 10.1038/s41598-023-30043-x

    View details for PubMedID 36810649

    View details for PubMedCentralID PMC9945466

  • Exploring disease interrelationships in patients with lymphatic disorders: A single center retrospective experience. Clinical and translational medicine Rockson, S. G., Zhou, X., Zhao, L., Hosseini, D. K., Jiang, X., Sweatt, A. J., Kim, D., Tian, W., Snyder, M. P., Nicolls, M. R. 2022; 12 (4): e760

    Abstract

    The lymphatic contribution to the circulation is of paramount importance in regulating fluid homeostasis, immune cell trafficking/activation and lipid metabolism. In comparison to the blood vasculature, the impact of the lymphatics has been underappreciated, both in health and disease, likely due to a less well-delineated anatomy and function. Emerging data suggest that lymphatic dysfunction can be pivotal in the initiation and development of a variety of diseases across broad organ systems. Understanding the clinical associations between lymphatic dysfunction and non-lymphatic morbidity provides valuable evidence for future investigations and may foster the discovery of novel biomarkers and therapies.We retrospectively analysed the electronic medical records of 724 patients referred to the Stanford Center for Lymphatic and Venous Disorders. Patients with an established lymphatic diagnosis were assigned to groups of secondary lymphoedema, lipoedema or primary lymphovascular disease. Individuals found to have no lymphatic disorder were served as the non-lymphatic controls. The prevalence of comorbid conditions was enumerated. Pairwise co-occurrence pattern analyses, validated by Jaccard similarity tests, was utilised to investigate disease-disease interrelationships.Comorbidity analyses underscored the expected relationship between the presence of secondary lymphoedema and those diseases that damage the lymphatics. Cardiovascular conditions were common in all lymphatic subgroups. Additionally, statistically significant alteration of disease-disease interrelationships was noted in all three lymphatic categories when compared to the control population.The presence or absence of a lymphatic disease significantly influences disease interrelationships in the study cohorts. As a physiologic substrate, the lymphatic circulation may be an underappreciated participant in disease pathogenesis. These relationships warrant further, prospective scrutiny and study.

    View details for DOI 10.1002/ctm2.760

    View details for PubMedID 35452183

  • Pathophysiology of the Lymphatic System in Patients With HeartFailure: JACC State-of-the-Art Review. Journal of the American College of Cardiology Itkin, M., Rockson, S. G., Burkhoff, D. 2021; 78 (3): 278-290

    Abstract

    The removal of interstitial fluid from the tissues is performed exclusively by the lymphatic system. Tissue edema in congestive heart failure occurs only when the lymphatic system fails or is overrun by fluid leaving the vascular space across the wall of the capillaries into the interstitial space. This process is driven by Starling forces determined by hydrostatic and osmotic pressures and organ-specific capillary permeabilities to proteins of different sizes. In this review, we summarize current knowledge of the generation of lymph in different organs, the mechanics by which lymph is returned to the circulation, and the consequences of the inadequacy of lymph flow. We review recent advances in imaging techniques that have allowed for new research, diagnostic, and therapeutic approaches to the lymphatic system. Finally, we review how efforts to increase lymph flow have demonstrated potential as a viable therapeutic approach for refractory heart failure.

    View details for DOI 10.1016/j.jacc.2021.05.021

    View details for PubMedID 34266581

  • Advances in Lymphedema. Circulation research Rockson, S. G. 2021; 128 (12): 2003-2016

    Abstract

    Lymphedema is a common, complex, and inexplicably underappreciated human disease. Despite a history of relative neglect by health care providers and by governmental health care agencies, the last decade has seen an explosive growth of insights into, and approaches to, the problem of human lymphedema. The current review highlights the significant advances that have occurred in the investigative and clinical approaches to lymphedema, particularly over the last decade. This review summarizes the progress that has been attained in the realms of genetics, lymphatic imaging, and lymphatic surgery. Newer molecular insights are explored, along with their relationship to future molecular therapeutics. Growing insights into the relationships among lymphedema, obesity, and other comorbidities are important to consider in current and future responses to patients with lymphedema.

    View details for DOI 10.1161/CIRCRESAHA.121.318307

    View details for PubMedID 34110905

  • Leukotrienes in Tumor-Associated Inflammation. Frontiers in pharmacology Tian, W., Jiang, X., Kim, D., Guan, T., Nicolls, M. R., Rockson, S. G. 2020; 11: 1289

    Abstract

    Leukotrienes are biologically active eicosanoid lipid mediators that originate from oxidative metabolism of arachidonic acid. Biosynthesis of leukotrienes involves a set of soluble and membrane-bound enzymes that constitute a machinery complex primarily expressed by cells of myeloid origin. Leukotrienes and their synthetic enzymes are critical immune modulators for leukocyte migration. Increased concentrations of leukotrienes are implicated in a number of inflammatory disorders. More recent work indicates that leukotrienes may also interact with a variety of tissue cells, contributing to the low-grade inflammation of cardiovascular, neurodegenerative, and metabolic conditions, as well as that of cancer. Leukotriene signaling contributes to the active tumor microenvironment, promoting tumor growth and resistance to immunotherapy. This review summarizes recent insights into the intricate roles of leukotrienes in promoting tumor growth and metastasis through shaping the tumor microenvironment. The emerging possibilities for pharmacological targeting of leukotriene signaling in tumor metastasis are considered.

    View details for DOI 10.3389/fphar.2020.01289

    View details for PubMedID 32973519

    View details for PubMedCentralID PMC7466732

  • Platelet factor 4 is a biomarker for lymphatic-promoted disorders. JCI insight Ma, W. n., Gil, H. J., Escobedo, N. n., Benito-Martín, A. n., Ximénez-Embún, P. n., Muñoz, J. n., Peinado, H. n., Rockson, S. G., Oliver, G. n. 2020

    Abstract

    Genetic or acquired defects of the lymphatic vasculature often result in disfiguring, disabling and, occasionally, life-threatening clinical consequences. Advanced forms of lymphedema are readily diagnosed clinically, but more subtle presentations often require invasive imaging or other technologies for a conclusive diagnosis. On the other hand, lipedema, a chronic lymphatic microvascular disease with pathological accumulation of subcutaneous adipose tissue is often misdiagnosed as obesity or lymphedema; currently there are no biomarkers or imaging criteria available for a conclusive diagnosis. Recent evidence suggests that otherwise asymptomatic defective lymphatic vasculature likely contributes to an array of other pathologies, including obesity, inflammatory bowel disease and neurological disorders, among others. Accordingly, identification of biomarkers of lymphatic malfunction will provide a valuable resource for the diagnosis and clinical discrimination of lymphedema, lipedema, obesity and other potential lymphatic-related pathologies. In this paper we profiled and compared blood plasma exosomes isolated from mouse models and from human subjects with and without symptomatic lymphatic pathologies. We identified platelet factor 4 (PF4/CXCL4) as a biomarker that could be used to diagnose lymphatic vasculature dysfunction. Furthermore, we determined that PF4 levels in circulating blood plasma exosomes were also elevated in lipedema patients, supporting current claims arguing that at least some of the underlying attributes of this disease are also the consequence of lymphatic defects.

    View details for DOI 10.1172/jci.insight.135109

    View details for PubMedID 32525843

  • Novel mutations in PIEZO1 cause an autosomal recessive generalized lymphatic dysplasia with non-immune hydrops fetalis (vol 6, 8035, 2015) NATURE COMMUNICATIONS Fotiou, E., Martin-Almedina, S., Simpson, M. A., Lin, S., Gordon, K., Brice, G., Atton, G., Jeffery, I., Rees, D. C., Mignot, C., Vogt, J., Homfray, T., Snyder, M. P., Rockson, S. G., Jeffery, S., Mortimer, P. S., Mansour, S., Ostergaard, P. 2019; 10
  • Cancer-associated secondary lymphoedema. Nature reviews. Disease primers Rockson, S. G., Keeley, V., Kilbreath, S., Szuba, A., Towers, A. 2019; 5 (1): 22

    Abstract

    Lymphoedema is an oedematous condition with a specific and complex tissue biology. In the clinical context of cancer, the pathogenesis of lymphoedema ensues most typically from the modalities employed to stage and treat the cancer (in particular, surgery and radiotherapy). Despite advances in cancer treatment, lifelong lymphoedema (limb swelling and the accompanying chronic inflammatory processes) affects approximately one in seven individuals treated for cancer, although estimates of lymphoedema prevalence following cancer treatment vary widely depending upon the diagnostic criteria used and the duration of follow-up. The natural history of cancer-associated lymphoedema is defined by increasing limb girth, fibrosis, inflammation, abnormal fat deposition and eventual marked cutaneous pathology, which also increases the risk of recurrent skin infections. Lymphoedema can substantially affect the daily quality of life of patients, as, in addition to aesthetic concerns, it can cause discomfort and affect the ability to carry out daily tasks. Clinical diagnosis is dependent on comparison of the affected region with the equivalent region on the unaffected side and, if available, with pre-surgical measurements. Surveillance is indicated in this high-risk population to facilitate disease detection at the early stages, when therapeutic interventions are most effective. Treatment modalities include conservative physical strategies that feature complex decongestive therapy (including compression garments) and intermittent pneumatic compression, as well as an emerging spectrum of surgical interventions, including liposuction for late-stage disease. The future application of pharmacological and microsurgical therapeutics for cancer-associated lymphoedema holds great promise.

    View details for DOI 10.1038/s41572-019-0072-5

    View details for PubMedID 30923312

  • Cancer-associated secondary lymphoedema NATURE REVIEWS DISEASE PRIMERS Rockson, S. G., Keeley, V., Kilbreath, S., Szuba, A., Towers, A. 2019; 5
  • Lymphedema after Breast Cancer Treatment NEW ENGLAND JOURNAL OF MEDICINE Rockson, S. G. 2018; 379 (20): 1937–44
  • Pilot studies demonstrate the potential benefits of antiinflammatory therapy in human lymphedema JCI INSIGHT Rockson, S. G., Tian, W., Jiang, X., Kuznetsova, T., Haddad, F., Zampell, J., Mehrara, B., Sampson, J. P., Roche, L., Kim, J., Nicolls, M. R. 2018; 3 (20)
  • Pilot studies demonstrate the potential benefits of antiinflammatory therapy in human lymphedema. JCI insight Rockson, S. G., Tian, W. n., Jiang, X. n., Kuznetsova, T. n., Haddad, F. n., Zampell, J. n., Mehrara, B. n., Sampson, J. P., Roche, L. n., Kim, J. n., Nicolls, M. R. 2018; 3 (20)

    Abstract

    Lymphedema is a common condition affecting millions around the world that still lacks approved medical therapy. Because ketoprofen, an NSAID, has been therapeutic in experimental lymphedema, we evaluated its efficacy in humans.We first performed an exploratory open-label trial. Patients with either primary or secondary lymphedema received ketoprofen 75 mg by mouth 3 times daily for 4 months. Subjects were evaluated for changes in histopathology, with skin thickness, limb volume, and tissue bioimpedance changes serving as secondary endpoints. Based on our encouraging findings, we next conducted a placebo-controlled trial, with the primary outcome defined as a change in skin thickness, as measured by skin calipers. Secondary endpoints for this second study included histopathology, limb volume, bioimpedance, and systemic inflammatory mediators.We enrolled 21 lymphedema patients in the open-label trial, from November 2010 to July 2011. Histopathology and skin thickness were significantly improved at 4 months compared with baseline. In the follow-up, double-blind, placebo-controlled trial, we enrolled 34 patients from August 2011 to October 2015, with 16 ketoprofen recipients and 18 placebo-treated subjects. No serious adverse events occurred. The ketoprofen recipients demonstrated reduced skin thickness, as well as improved composite measures of histopathology and decreased plasma granulocyte CSF (G-CSF) expression.These 2 exploratory studies together support the utility of targeted antiinflammatory therapy with ketoprofen in patients with lymphedema. Our results highlight the promise of such approaches to help restore a failing lymphatic circulation.ClinicalTrials.gov NCT02257970.

    View details for PubMedID 30333315

  • Leukotriene B-4 antagonism ameliorates experimental lymphedema SCIENCE TRANSLATIONAL MEDICINE Tian, W., Rockson, S. G., Jiang, X., Kim, J., Begaye, A., Shuffle, E. M., Tu, A. B., Cribb, M., Nepiyushchikh, Z., Feroze, A. H., Zamanian, R. T., Dhillon, G. S., Voelkel, N. F., Peters-Golden, M., Kitajewski, J., Dixon, J. B., Nicolls, M. R. 2017; 9 (389)
  • Lymphatic Dysfunction, Leukotrienes, and Lymphedema. Annual review of physiology Jiang, X. n., Nicolls, M. R., Tian, W. n., Rockson, S. G. 2017

    Abstract

    The lymphatic system is essential for the maintenance of tissue fluid homeostasis, gastrointestinal lipid absorption, and immune trafficking. Whereas lymphatic regeneration occurs physiologically in wound healing and tissue repair, pathological lymphangiogenesis has been implicated in a number of chronic diseases such as lymphedema, atherosclerosis, and cancer. Insight into the regulatory mechanisms of lymphangiogenesis and the manner in which uncontrolled inflammation promotes lymphatic dysfunction is urgently needed to guide the development of novel therapeutics: These would be designed to reverse lymphatic dysfunction, either primary or acquired. Recent investigation has demonstrated the mechanistic role of leukotriene B4 (LTB4) in the molecular pathogenesis of lymphedema. LTB4, a product of the innate immune response, is a constituent of the eicosanoid inflammatory mediator family of molecules that promote both physiological and pathological inflammation. Here we provide an overview of lymphatic development, the pathophysiology of lymphedema, and the role of leukotrienes in lymphedema pathogenesis. Expected final online publication date for the Annual Review of Physiology Volume 80 is February 10, 2018. Please see http://www.annualreviews.org/page/journal/pubdates for revised estimates.

    View details for PubMedID 29029593

  • Aligned nanofibrillar collagen scaffolds - Guiding lymphangiogenesis for treatment of acquired lymphedema. Biomaterials Hadamitzky, C., Zaitseva, T. S., Bazalova-Carter, M., Paukshto, M. V., Hou, L., Strassberg, Z., Ferguson, J., Matsuura, Y., Dash, R., Yang, P. C., Kretchetov, S., Vogt, P. M., Rockson, S. G., Cooke, J. P., Huang, N. F. 2016; 102: 259-267

    Abstract

    Secondary lymphedema is a common disorder associated with acquired functional impairment of the lymphatic system. The goal of this study was to evaluate the therapeutic efficacy of aligned nanofibrillar collagen scaffolds (BioBridge) positioned across the area of lymphatic obstruction in guiding lymphatic regeneration. In a porcine model of acquired lymphedema, animals were treated with BioBridge scaffolds, alone or in conjunction with autologous lymph node transfer as a source of endogenous lymphatic growth factor. They were compared with a surgical control group and a second control group in which the implanted BioBridge was supplemented with exogenous vascular endothelial growth factor-C (VEGF-C). Three months after implantation, immunofluorescence staining of lymphatic vessels demonstrated a significant increase in lymphatic collectors within close proximity to the scaffolds. To quantify the functional impact of scaffold implantation, bioimpedance was used as an early indicator of extracellular fluid accumulation. In comparison to the levels prior to implantation, the bioimpedance ratio was significantly improved only in the experimental BioBridge recipients with or without lymph node transfer, suggesting restoration of functional lymphatic drainage. These results further correlated with quantifiable lymphatic collectors, as visualized by contrast-enhanced computed tomography. They demonstrate the therapeutic potential of BioBridge scaffolds in secondary lymphedema.

    View details for DOI 10.1016/j.biomaterials.2016.05.040

    View details for PubMedID 27348849

  • The Cutaneous, Net Clinical, and Health Economic Benefits of Advanced Pneumatic Compression Devices in Patients With Lymphedema JAMA DERMATOLOGY Karaca-Mandic, P., Hirsch, A. T., Rockson, S. G., Ridner, S. H. 2015; 151 (11): 1187-1193

    Abstract

    The prevalence and clinical burden of lymphedema is known to be increasing. Nevertheless, evidence-based comparative effectiveness data regarding lymphedema therapeutic interventions have been poor.To examine the impact of an advanced pneumatic compression device (APCD) on cutaneous and other clinical outcomes and health economic costs in a representative privately insured population of lymphedema patients.Retrospective analysis of a deidentified private insurance database from 2007 through 2013, and multivariate regression analysis comparing outcomes for the 12 months before and after APCD purchase, adjusting for baseline patient characteristics. Patients with lymphedema who received an APCD who were commercially insured and Medicare managed care enrollees from a large, national US managed care health insurer. The study population was evaluated as cancer-related and non-cancer-related lymphedema cohorts.Receipt of an APCD.Rates of cellulitis, use of lymphedema-related manual therapy, outpatient hospital visits, and inpatient hospitalizations. Lymphedema-related direct costs were measured for home health care, hospital outpatient care, office visits, emergency department use, and inpatient care.The study sample included 718 patients (374 in the cancer cohort and 344 in the noncancer cohort). In both cohorts, use of an APCD was associated with similar reductions in adjusted rates of cellulitis episodes (from 21.1% to 4.5% in the cancer cohort and 28.8% to 7.3% in the noncancer cohort; P < .001 for both), lymphedema-related manual therapy (from 35.6% to 24.9%in the cancer cohort and 32.3% to 21.2% in the noncancer cohort; P < .001 for both), and outpatient visits (from 58.6% to 41.4% in the cancer cohort and 52.6% to 31.4% in the noncancer cohort; P < .001 for both). Among the cancer cohort, total lymphedema-related costs per patient, excluding medical equipment costs, were reduced by 37% (from $2597 to $1642, P = .002). The corresponding decline in costs for the noncancer cohort was 36% (from $2937 to $1883, P = .007).The study found an association between significant reductions in episodes of cellulitis (cancer vs noncancer cohorts) and outpatient care and costs of APCD acquisition within a 1-year time frame in patients with both cancer-related and non-cancer-related lymphedema.

    View details for DOI 10.1001/jamadermatol.2015.1895

    View details for PubMedID 26444458

  • Novel mutations in PIEZO1 cause an autosomal recessive generalized lymphatic dysplasia with non-immune hydrops fetalis. Nature communications Fotiou, E., Martin-Almedina, S., Simpson, M. A., Lin, S., Gordon, K., Brice, G., Atton, G., Jeffery, I., Rees, D. C., Mignot, C., Vogt, J., Homfray, T., Snyder, M. P., Rockson, S. G., Jeffery, S., Mortimer, P. S., Mansour, S., Ostergaard, P. 2015; 6: 8085-?

    Abstract

    Generalized lymphatic dysplasia (GLD) is a rare form of primary lymphoedema characterized by a uniform, widespread lymphoedema affecting all segments of the body, with systemic involvement such as intestinal and/or pulmonary lymphangiectasia, pleural effusions, chylothoraces and/or pericardial effusions. This may present prenatally as non-immune hydrops. Here we report homozygous and compound heterozygous mutations in PIEZO1, resulting in an autosomal recessive form of GLD with a high incidence of non-immune hydrops fetalis and childhood onset of facial and four limb lymphoedema. Mutations in PIEZO1, which encodes a mechanically activated ion channel, have been reported with autosomal dominant dehydrated hereditary stomatocytosis and non-immune hydrops of unknown aetiology. Besides its role in red blood cells, our findings indicate that PIEZO1 is also involved in the development of lymphatic structures.

    View details for DOI 10.1038/ncomms9085

    View details for PubMedID 26333996

  • Laboratory models for the investigation of lymphangiomatosis MICROVASCULAR RESEARCH Rockson, S. G. 2014; 96: 64-67

    Abstract

    Lymphangiomatosis is an uncommon proliferative disorder of the lymphatic vasculature whose etiology remains poorly understood. The lymphangiomatosis spectrum encompasses a remarkable heterogeneity in its potential presentation, including micro- and macrocystic isolated lymphatic malformations, thoracic and intraabdominal diffuse lymphangiomatosis, and osseous and soft-tissue presentations known as Gorham-Stout disease. Recent therapeutic advances are empirical in nature or, at best, inferential, reflecting the scanty availability of laboratory-based model systems for the mechanistic study of this disease. Several promising model systems are reviewed here. The laboratory investigation of lymphangiomatosis will likely continue to benefit from the remarkable growth of insights into the mechanisms of lymphangiogenesis and vascular development.

    View details for DOI 10.1016/j.mvr.2014.08.007

    View details for PubMedID 25173588

  • New developments in clinical aspects of lymphatic disease JOURNAL OF CLINICAL INVESTIGATION Mortimer, P. S., Rockson, S. G. 2014; 124 (3): 915-921

    Abstract

    The lymphatic system is fundamentally important to cardiovascular disease, infection and immunity, cancer, and probably obesity--the four major challenges in healthcare in the 21st century. This Review will consider the manner in which new knowledge of lymphatic genes and molecular mechanisms has demonstrated that lymphatic dysfunction should no longer be considered a passive bystander in disease but rather an active player in many pathological processes and, therefore, a genuine target for future therapeutic developments. The specific roles of the lymphatic system in edema, genetic aspects of primary lymphedema, infection (cellulitis/erysipelas), Crohn's disease, obesity, cancer, and cancer-related lymphedema are highlighted.

    View details for DOI 10.1172/JCI71608

    View details for Web of Science ID 000332347700006

    View details for PubMedID 24590276

    View details for PubMedCentralID PMC3938261

  • Lymphedema prevalence and treatment benefits in cancer: impact of a therapeutic intervention on health outcomes and costs. PloS one Brayton, K. M., Hirsch, A. T., O Brien, P. J., Cheville, A., Karaca-Mandic, P., Rockson, S. G. 2014; 9 (12)

    Abstract

    Lymphedema is a common complication of cancer therapeutics; its prevalence, treatment outcomes, and costs have been poorly defined. The objective of this study was to examine lymphedema prevalence among cancer survivors and to characterize changes in clinical outcomes and costs associated with a defined therapeutic intervention (use of a pneumatic compression devices [PCD]) in a representative, privately insured population.Retrospective analysis of de-identified health claims data from a large national insurer for calendar years 2007 through 2013. Patients were required to have 12 months of continuous insurance coverage prior to PCD receipt (baseline), as well as a 12-month follow-up period. Analyses were performed for individuals with cancer-related lymphedema (n = 1,065). Lymphedema prevalence was calculated: number of patients with a lymphedema claim in a calendar year divided by total number of enrollees. The impact of PCD use was evaluated by comparing rates of a pre-specified set of health outcomes and costs for the 12 months before and after, respectively, PCD receipt. Lymphedema prevalence among cancer survivors increased from 0.95% in 2007 to 1.24% in 2013. PCD use was associated with decreases in rates of hospitalizations (45% to 32%, p<0.0001), outpatient hospital visits (95% to 90%, p<0.0001), cellulitis diagnoses (28% to 22%, p = 0.003), and physical therapy use (50% to 41%, p<0.0001). The average baseline health care costs were high ($53,422) but decreased in the year after PCD acquisition (-$11,833, p<0.0001).Lymphedema is a prevalent medical condition that is often a defining attribute of cancer survivorship. The problem is associated with high health care costs; Treatment (in this instance, use of PCD) is associated with significant decreases in adverse clinical outcomes and costs.

    View details for DOI 10.1371/journal.pone.0114597

    View details for PubMedID 25470383

  • The Lymphatics and the Inflammatory Response: Lessons Learned from Human Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2013; 11 (3): 117-120

    Abstract

    In lymphedema, there is a profound predisposition to infection with bacterial pathogens. It therefore seems appropriate to reconsider our unique functional definition of the lymphatic structures within a circulatory construct. While the lymphatics unquestionably fulfill a vital circulatory function, it seems more appropriate to view this complex network, comprised both of endothelial-lined vessels and of lymphoid tissue, as the nexus between the circulatory and immune systems. Viewed in this fashion, it becomes evident that the complex biology of regional lymphatic disruption is a manifestation of the interplay between these two vital bodily functions. Experimental lymph stasis in murine model has been utilized to effectively demonstrate the pathological attributes of human lymphedema, namely, inflammation, fat deposition, and fibrosis. Large-scale transcriptional corroborates the role of inflammatory mechanisms. The murine studies have set the stage for subsequent translational investigation of human lymphedema. Many of the gene expression pathways invoked by lymphedema are relevant to the inflammatory response and have provided a pragmatic approach to the successful identification of potentially relevant circulating biomarkers for human lymphedema.

    View details for DOI 10.1089/lrb.2013.1132

    View details for PubMedID 24024576

  • Prospective Transcriptomic Pathway Analysis of Human Lymphatic Vascular Insufficiency: Identification and Validation of a Circulating Biomarker Panel PLOS ONE Lin, S., Kim, J., Lee, M., Roche, L., Yang, N. L., Tsao, P. S., Rockson, S. G. 2012; 7 (12)

    Abstract

    In our previous transcriptional profiling of a murine model, we have identified a remarkably small number of specific pathways with altered expression in lymphedema. In this investigation, we utilized microarray-based transcriptomics of human skin for an unbiased a priori prospective candidate identification, with subsequent validation of these candidates through direct serum assay. The resulting multi-analyte biomarker panel sensitively should sensitively discriminate human lymphedema subjects from normal individuals.We enrolled 63 lymphedema subjects and 27 normals in our attempt to discover protein analytes that can distinguish diseased individuals from controls. To minimize technical and biologically irrelevant variation, we first identified potential candidates by performing transcriptional microarray analysis on paired diseased and normal skin specimens sampled from the same individuals. We focused our attention on genes with corresponding protein products that are secreted and took these candidates forward to a protein multiplex assay applied to diseased and normal subjects. We developed a logistic regression-based model on an eventual group of six proteins and validated our system on a separate cohort of study subjects. The area under the receiver operating characteristic curve was calculated to be 0.87 (95% CI : 0.75 to 0.97).We have developed an accurate bioassay utilizing proteins representing four central pathogenetic modalities of the disease: lymphangiogenesis, inflammation, fibrosis, and lipid metabolism, suggesting that these proteins are directly related to the pathogenesis of the tissue pathology in lymphatic vascular insufficiency. Further studies are warranted to determine whether this newly-identified biomarker panel will possess utility as an instrument for in vitro diagnosis of early and latent disease; the ultimate applicability to risk stratification, quantitation of disease burden, and response to therapy can easily be envisioned.

    View details for DOI 10.1371/journal.pone.0052021

    View details for PubMedID 23272198

  • Lower Extremity Cancers LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Lee, M., Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 507–13
  • Medical Treatment LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 273–75
  • Physiology, Pathophysiology, and Lymphodynamics: General Overview LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 59–61
  • Lymphodynamics LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 63–64
  • Etiology and Classification of Lymphatic Disorders LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 11–28
  • Compression Therapy LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 251–55
  • Intermittent Pneumatic Compression Therapy LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 257–61
  • Head and Neck Lymphedema LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Vaillant-Newman, A., Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 295–306
  • Genetic Prospects for Lymphedema Management LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 491–97
  • Anti-Inflammatory Pharmacotherapy with Ketoprofen Ameliorates Experimental Lymphatic Vascular Insufficiency in Mice PLOS ONE Nakamura, K., Radhakrishnan, K., Wong, Y. M., Rockson, S. G. 2009; 4 (12)

    Abstract

    Disruption of the lymphatic vasculature causes edema, inflammation, and end-tissue destruction. To assess the therapeutic efficacy of systemic anti-inflammatory therapy in this disease, we examined the impact of a nonsteroidal anti-inflammatory drug (NSAID), ketoprofen, and of a soluble TNF-alpha receptor (sTNF-R1) upon tumor necrosis factor (TNF)-alpha activity in a mouse model of acquired lymphedema.Lymphedema was induced by microsurgical ablation of major lymphatic conduits in the murine tail. Untreated control mice with lymphedema developed significant edema and extensive histopathological inflammation compared to sham surgical controls. Short-term ketoprofen treatment reduced tail edema and normalized the histopathology while paradoxically increasing TNF-alpha gene expression and cytokine levels. Conversely, sTNF-R1 treatment increased tail volume, exacerbated the histopathology, and decreased TNF-alpha gene expression. Expression of vascular endothelial growth factor-C (VEGF-C), which stimulates lymphangiogenesis, closely correlated with TNF-alpha expression.Ketoprofen therapy reduces experimental post-surgical lymphedema, yet direct TNF-alpha inhibition does not. Reducing inflammation while preserving TNF-alpha activity appears to optimize the repair response. It is possible that the observed favorable responses, at least in part, are mediated through enhanced VEGF-C signaling.

    View details for DOI 10.1371/journal.pone.0008380

    View details for PubMedID 20027220

  • Therapeutic responses to exogenous VEGF-C administration in experimental lymphedema: immunohistochemical and molecular characterization. Lymphatic research and biology Jin, D. P., An, A., Liu, J., Nakamura, K., Rockson, S. G. 2009; 7 (1): 47-57

    Abstract

    In a widely employed murine tail model of human acquired lymphedema, we have previously observed that, distal to the site of experimental lymphatic ablation, there is immunohistochemical evidence of a profound increase in cutaneous lymphatic vessel number and size that normalizes after VEGF-C administration.In order to investigate the mechanistic basis of the lymphatic microvascular remodeling, we have studied the lymphedematous responses to VEGF-C after co-administration of systemic VEGFR-3 neutralizing antibody. We have also undertaken genome-wide whole-tissue transcriptional profiling of lymphedematous tissues before and after exogenous VEGF-C administration.We provoked postsurgical lymphedema in the mouse tail model and assessed the effects of exogenously administered human recombinant VEGF-C in the presence of a monoclonal anti-VEGFR-3 antibody. Polyclonal IgG was administered to a series of control subjects. Microvascular lymphatic remodeling was assessed through quantitative and qualitative anti-LYVE1 immunohistochemistry. Genome-wide transcriptional profiling was performed in whole skin derived from lymphedema with and without exogenous VEGF-C administration. Normal mice and surgical shams served as controls.In the presence of the monoclonal anti-VEGFR-3 neutralizing antibody, positive lymphatic microvascular remodeling in lymphedematous skin is nearly completely abrogated. Furthermore, the therapeutic impact of added VEGF-C is markedly attenuated, as is the ability of the growth factor to ameliorate tissue edema. Transcriptional profiling of the VEGF-C responses in treated lymphedema reveals a very restricted list of genes whose expression is upregulated in lymphedema and re-normalized following VEGF-C treatment.The postsurgical murine tail model of lymphedema closely simulates attributes of human lymphedema. The current series of investigations underscores the utility of the murine tail model to the preclinical and translational investigation of lymphedema. The derived insights continue to focus favorably upon the central role of the VEGFR-3 receptor and its ligands in the development and therapeutic resolution of lymphedema. Whole tissue transcriptional profiling continues to shed light on disease mechanisms and potential future targets for therapeutic intervention.

    View details for DOI 10.1089/lrb.2009.0002

    View details for PubMedID 19302023

  • The role of the lymphatic circulation in the natural history and expression of cardiovascular disease INTERNATIONAL JOURNAL OF CARDIOLOGY Nakamura, K., Rockson, S. G. 2008; 129 (3): 309-317

    Abstract

    The lymphatic vasculature is essential to fluid, protein and cellular transport, and to immune responsiveness. The last decade has witnessed a virtual renaissance of investigation into the function of the lymphatic microvasculature, prompting re-consideration of its role in the genesis and progression of cardiovascular pathology. The lymphatic microvasculature of the heart and vascular wall likely participate in atherogenesis, myocardial infarction, congestive heart failure, and cardiac transplantation. Intensive exploration of lymphatic mechanisms of cardiovascular disease is likely to lead to enhanced insights and novel therapeutic approaches.

    View details for DOI 10.1016/j.ijcard.2008.02.007

    View details for PubMedID 18559287

  • Diagnosis and management of lymphatic vascular disease JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY Rockson, S. G. 2008; 52 (10): 799-806

    Abstract

    The lymphatic vasculature is comprised of a network of vessels that is essential both to fluid homeostasis and to the mediation of regional immune responses. In health, the lymphatic vasculature possesses the requisite transport capacity to accommodate the fluid load placed upon it. The most readily recognizable attribute of lymphatic vascular incompetence is the presence of the characteristic swelling of tissues, called lymphedema, which arises as a consequence of insufficient lymph transport. The diagnosis of lymphatic vascular disease relies heavily upon the physical examination. If the diagnosis remains in question, the presence of lymphatic vascular insufficiency can be ascertained through imaging, including indirect radionuclide lymphoscintigraphy. Beyond lymphoscintigraphy, clinically-relevant imaging modalities include magnetic resonance imaging and computerized axial tomography. The state-of-the-art therapeutic approach to lymphatic edema relies upon physiotherapeutic techniques. Complex decongestive physiotherapy is an empirically-derived, effective, multicomponent technique designed to reduce limb volume and maintain the health of the skin and supporting structures. The application of pharmacological therapies has been notably absent from the management strategies for lymphatic vascular insufficiency states. In general, drug-based approaches have been controversial at best. Surgical approaches to improve lymphatic flow through vascular reanastomosis have been, in large part, unsuccessful, but controlled liposuction affords lasting benefit in selected patients. In the future, specifically engineered molecular therapeutics may be designed to facilitate the controlled regrowth of damaged, dysfunctional, or obliterated lymphatic vasculature in order to circumvent or mitigate the vascular insufficiency that leads to edema and tissue destruction.

    View details for DOI 10.1016/j.jacc.2008.06.005

    View details for PubMedID 18755341

  • The clinical spectrum of lymphatic disease LYMPHATIC CONTINUUM REVISITED Radhakrisihnan, K., Rockson, S. G. 2008; 1131: 155-184

    Abstract

    Lymphatic disease is quite prevalent, and often not well clinically characterized. Beyond lymphedema, there is a broad array of human disease that directly or indirectly alters lymphatic structure and function. The symptomatic and objective presentation of these patients can be quite diverse. In this review, we have attempted to provide a systematic overview of the subjective and objective spectrum of lymphatic disease, with consideration of all of the categories of disease that primarily or secondarily impair the functional integrity of the lymphatic system. Lymphedema is discussed, along with chromosomal disorders, lymphangioma, infectious diseases, lymphangioleiomyomatosis, lipedema, heritable genetic disorders, complex vascular malformations, protein-losing enteropathy, and intestinal lymphangiectasia.

    View details for DOI 10.1196/annals.1413.015

    View details for PubMedID 18519969

  • Estimating the population burden of lymphedema LYMPHATIC CONTINUUM REVISITED Rockson, S. G., Rivera, K. K. 2008; 1131: 147-154

    Abstract

    Lymphedema is a complex, regional edematous state that ensues when lymph transport is insufficient to maintain tissue homeostasis. The disorder is remarkably prevalent, but the population implications of lymphatic dysfunction are not well-studied. Prevalence estimates for lymphedema are relatively high, yet its prevalence is likely underestimated. The ability to estimate the burden of disease poses profound implications for current and future lymphedema patients, but the challenge to correctly surmise the incidence and prevalence of lymphedema is complex and the relevant medical literature is scanty. In the absence of the highly desired, prospectively designed and rigorously performed relevant epidemiologic studies, it is instructive to look at the existing studies of lymphedema disease burden. In the current review, the extant literature is examined in the context of the disease setting in which tissue edema is encountered. Incidence or prevalence estimates are provided or inferred, and, where feasible, the size of the subject population is also identified. It is extremely attractive to contemplate that future approaches will entail formal, prospectively designed studies to objectively quantitate incidence and prevalence statistics for individual categories, as well as for the global lymphedema population.

    View details for DOI 10.1196/annals.1413.014

    View details for PubMedID 18519968

  • Animal models for the molecular and mechanistic study of lymphatic biology and disease LYMPHATIC CONTINUUM REVISITED Shin, W. S., Rockson, S. G. 2008; 1131: 50-74

    Abstract

    The development of animal model systems for the study of the lymphatic system has resulted in an explosion of information regarding the mechanisms governing lymphatic development and the diseases associated with lymphatic dysfunction. Animal studies have led to a new molecular model of embryonic lymphatic vascular development, and have provided insight into the pathophysiology of both inherited and acquired lymphatic insufficiency. It has become apparent, however, that the importance of the lymphatic system to human disease extends, beyond its role in lymphedema, to many other diverse pathologic processes, including, very notably, inflammation and tumor lymphangiogenesis. Here, we have undertaken a systematic review of the models as they relate to molecular and functional characterization of the development, maturation, genetics, heritable and acquired diseases, and neoplastic implications of the lymphatic system. The translation of these advances into therapies for human diseases associated with lymphatic dysfunction will require the continued study of the lymphatic system through robust animal disease models that simulate their human counterparts.

    View details for DOI 10.1196/annals.1413.005

    View details for PubMedID 18519959

  • Biomarkers of lymphatic function and disease: state of the art and future directions. Molecular diagnosis & therapy Nakamura, K., Rockson, S. G. 2007; 11 (4): 227-238

    Abstract

    Substantial advances have accrued over the last decade in the identification of the processes that contribute to lymphatic vascular development in health and disease. Identification of distinct regulatory milestones, from a variety of genetic models, has led to a stepwise chronology of lymphatic development. Several molecular species have been identified as important tissue biomarkers of lymphatic development and function. At present, vascular endothelial growth-factor receptor (VEGFR)-3/VEGF-C/VEGF-D signaling has proven useful in the identification of clinical lymphatic metastatic potential and the assessment of cancer prognosis. Similar biomarkers, to be utilized as surrogates for the assessment of inherited and acquired diseases of the lymphatic circulation, are actively sought, and will represent a signal advance in biomedical investigation.

    View details for PubMedID 17705577

  • Inflammatory manifestations of experimental lymphatic insufficiency PLOS MEDICINE Tabibiazar, R., Cheung, L., Han, J., Swanson, J., Beilhack, A., An, A., Dadras, S. S., Rockson, N., Joshi, S., Wagner, R., Rockson, S. G. 2006; 3 (7): 1114-1139

    Abstract

    Sustained lymph stagnation engenders a pathological response that is complex and not well characterized. Tissue inflammation in lymphedema may reflect either an active or passive consequence of impaired immune traffic.We studied an experimental model of acute post-surgical lymphedema in the tails of female hairless, immunocompetent SKH-1 mice. We performed in vivo imaging of impaired immune traffic in experimental, murine acquired lymphatic insufficiency. We demonstrated impaired mobilization of immunocompetent cells from the lymphedematous region. These findings correlated with histopathological alterations and large-scale transcriptional profiling results. We found intense inflammatory changes in the dermis and the subdermis. The molecular pattern in the RNA extracted from the whole tissue was dominated by the upregulation of genes related to acute inflammation, immune response, complement activation, wound healing, fibrosis, and oxidative stress response.We have characterized a mouse model of acute, acquired lymphedema using in vivo functional imaging and histopathological correlation. The model closely simulates the volume response, histopathology, and lymphoscintigraphic characteristics of human acquired lymphedema, and the response is accompanied by an increase in the number and size of microlymphatic structures in the lymphedematous cutaneous tissues. Molecular characterization through clustering of genes with known functions provides insights into processes and signaling pathways that compose the acute tissue response to lymph stagnation. Further study of genes identified through this effort will continue to elucidate the molecular mechanisms and lead to potential therapeutic strategies for lymphatic vascular insufficiency.

    View details for DOI 10.1371/journal.pmed.0030254

    View details for PubMedID 16834456

  • A pilot, prospective evaluation of a novel alternative for maintenance therapy of breast cancer-associated lymphedema [ISRCTN76522412] BMC CANCER Wilburn, O., Wilburn, P., Rockson, S. G. 2006; 6

    Abstract

    Prospective investigations of complete decongestive lymphatic physiotherapy (CDPT), including manual lymphatic drainage (MLD), have validated the efficacy of these interventions for the initial reduction of edema and long-term maintenance of limb volume in lymphedema. However, CDPT demands substantial time and effort from patients to maintain these benefits; the treatments are not always well-accepted, and patients may suffer from a deterioration in quality-of-life or a time-dependent loss of initial treatment benefits. A new device designed for home use by the patient, the Flexitouch, has been developed to mechanically simulate MLD. We have undertaken a prospective, randomized, crossover study of the efficacy of the Flexitouch, when compared to massage, in the self-administered maintenance therapy of lymphedema.A prospective, randomized, crossover study of maintenance therapy was performed in 10 patients with unilateral breast cancer-associated lymphedema of the arm. Each observation phase included self-administered treatment with the Flexitouch or massage, 1 hour daily for 14 days, respectively, followed by crossover to the alternate treatment phase. Each treatment phase was preceded by a 1 week treatment washout, with use of garment only. The sequence of treatment was randomly assigned. The potential impact of treatment modality on quality of life was assessed with serial administration of the SF-36.Statistical analysis disclosed that the order of treatment had no outcome influence, permitting 10 comparisons within each treatment group. Post-treatment arm volume reduced significantly after the Flexitouch, but not after self-administered massage. The patients' mean weight decreased significantly with Flexitouch use, but not with massage. The Flexitouch device was apparently well-tolerated and accepted by patients. Serial SF-36 administration showed no deterioration in physical or psychosocial scores compared to baseline measurements; there were no statistical differences in scores when the two treatment modalities were compared.This short-term prospective evaluation of the Flexitouch suggests that the device may provide better maintenance edema control than self-adiminstered massage in breast cancer-associated lymphedema. The apparent ease of use and reliability of response to the device suggest that further broad-scale testing is warranted.

    View details for DOI 10.1186/1471-2407-6-84

    View details for PubMedID 16571129

  • Validation of a new technique for the quantitation of edema in the experimental setting. Lymphatic research and biology Pan, D., Han, J., Wilburn, P., Rockson, S. G. 2006; 4 (3): 153-158

    Abstract

    An inherent limitation to the study of in vivo animal models of lymphedema is the potential inaccuracy or unreliability of existing methods for the quantification of edema volume as a surrogate functional measure of lymphatic transport capacity. Circumference-based techniques have been proposed and validated as a suitable alternative to volume displacement measurements in human clinical studies; accordingly, we have elaborated a new application of this approach that can be applied to small animal studies.Acute postsurgical lymphedema was created experimentally in the murine tail. Both normal and lymphedematous murine tails were examined. Tail volume was quantitated both by water displacement and by a digital photographic technique. In selected mice, after sacrificed on postsurgical day 7, a 6 cm segment was resected from the midportion of the tail and cauterized to create a closed space. Known incremental volumes of saline (20-100 microL) were injected for subsequent digital photographic volumetry.The coefficients of variation for volume assessment by water displacement and by digital imaging were 0.08+/-0.09 and 0.01+/-0.009, respectively. The two techniques were poorly correlated: while serial water displacement analysis yielded highly variable measurements within the same tail, concurrent digital imaging of the tail circumference was quite reproducible. Furthermore, after parenteral injection of known incremental volumes of saline, the correlation between the injectate volumes and the digitally measured increases in volume was high, both in the normal and the lymphedematous tail.In the murine tail, when compared to water displacement volumetry, digital photography yields highly reproducible data. We can conclude that the lack of correlation between the two methods, with the relatively flat slope of the linear regression relationship, reflects inherent inaccuracies of the water displacement method.

    View details for PubMedID 17034295

  • An experimental model for the study of lymphedema and its response to therapeutic lymphangiogenesis BIODRUGS Cheung, L., Han, J., Beilhack, A., Joshi, S., Wilburn, P., Dua, A., An, A., Rockson, S. G. 2006; 20 (6): 363-370

    Abstract

    Evaluation of the efficacy of molecular treatment strategies for lymphatic vascular insufficiency requires a suitable preclinical animal model. Ideally, the model should closely replicate the untreated human disease in its pathogenesis and pathological expression.We have undertaken a study of the time course of the development and resolution of acquired, experimental lymphedema and of its responses to vascular endothelial growth factor (VEGF)-C lymphangiogenesis in the mouse tail model.We provoked post-surgical lymphedema in the mouse tail model and assessed the effects of exogenously administered human recombinant VEGF-C. Quantitative assessment of immune traffic function was performed through sequential in vivo bioluminescent imaging.In untreated lymphedema, tail edema was sustained until day 21. Exogenous administration of human recombinant VEGF-C produced a significant decrease in volume. Untreated lymphedema in the mouse tail model was characterized by the presence of dilated cutaneous lymphatics, marked acute inflammatory changes, and hypercellularity; VEGF-C produced a substantial reversion to the normal pattern, with notable regression in the size and number of cutaneous lymphatic vessels that express lymphatic vessel endothelial hyaluronan receptor-1 (LYVE-1). In vivo imaging confirmed the presence of an impairment of immune traffic in lymphedema that was ameliorated after VEGF-C administration.The post-surgical murine tail model of lymphedema closely simulates attributes of human lymphedema and provides the requisite sensitivity to detect therapeutically induced functional and structural alterations. It can, therefore, be used as an investigative platform to assess mechanisms of disease and its responses to candidate therapies, such as therapeutic lymphangiogenesis.

    View details for PubMedID 17176124

  • Therapeutic lymphangiogenesis with human recombinant VEGF-C. FASEB journal Szuba, A., Skobe, M., Karkkainen, M. J., Shin, W. S., Beynet, D. P., Rockson, N. B., Dakhil, N., Spilman, S., Goris, M. L., Strauss, H. W., Quertermous, T., Alitalo, K., Rockson, S. G. 2002; 16 (14): 1985-1987

    Abstract

    Chronic regional impairments of the lymphatic circulation often lead to striking architectural abnormalities in the lymphedematous tissues. Lymphedema is a common, disabling disease that currently lacks a cure. Vascular endothelial growth factors C and D mediate lymphangiogenesis through the VEGFR-3 receptor on lymphatic endothelia. The purpose of this study was to investigate the therapeutic potential for lymphangiogenesis with VEGF-C. We developed a rabbit ear model to simulate human chronic postsurgical lymphatic insufficiency. Successful, sustained surgical ablation of the ear lymphatics was confirmed by water displacement volumetry. After complete healing, the experimental animals (n=8) received a single, s.c. 100 microg dose of VEGF-C in the operated ear; controls (n=8) received normal saline. Radionuclide lymphoscintigraphy was performed to quantitate lymphatic function. Immunohistochemistry (IHC) was performed 7-8 days following treatment. After VEGF-C, there was a quantifiable amelioration of lymphatic function. IHC confirmed a significant increase in lymphatic vascularity, along with reversal of the intense tissue hypercellularity of untreated lymphedema. This study confirms the capacity of a single dose of VEGF-C to induce therapeutic lymphangiogenesis in acquired lymphedema. In addition to improving lymphatic function and vascularity, VEGF-C can apparently reverse the abnormalities in tissue architecture that accompany chronic lymphatic insufficiency.

    View details for PubMedID 12397087

  • The influence of non-cancer-related risk factors on the development of cancer-related lymphedema: a rapid review. Medical oncology (Northwood, London, England) Stout, N. L., Dierkes, M., Oliveri, J. M., Rockson, S., Paskett, E. D. 2024; 41 (11): 274

    Abstract

    Extensive research supports an evidence-base for cancer treatment-related risk factors, including extent of lymph node dissection and use of radiotherapy, as contributing to secondary lymphedema. Additionally, comorbidities, such as higher body mass index, and vascular-related conditions are identified to further augment risk. While social determinants of health (SDOH) and socioeconomic factors are widely regarded as influencing an individual's healthcare outcomes, including cancer risk and survival, these factors have not been explored as risk factors for developing secondary lymphedema. A rapid literature review explored the current evidence for SDOH as risk factors for lymphedema. Studies that were published over the last 10 years and that specifically analyzed social factors as variables associated with lymphedema were included. Studies that only characterized the social determinants of the study population were not included. Forty-nine studies were identified through a rapid literature review, and 13 studies that expressly analyzed social determinants as risk factors for secondary lymphedema were reviewed and extracted. All studies were conducted in patients with breast cancer-related lymphedema. Social risk factors included race, educational level, insurance type, and income level. These are consistent with the socioeconomic inequalities related to cancer survival. SDOH may influence the risk of developing cancer treatment-related health conditions like secondary lymphedema. Research trials studying cancer treatment-related conditions should collect consistent and robust data across social, behavioral, environmental, and economic domains and should analyze these variables to understand their contribution to study endpoints. Risk prediction modeling could be a future pathway to better incorporate social determinants, along with medical and co-morbidity data, to holistically understand lymphedema risk.

    View details for DOI 10.1007/s12032-024-02474-7

    View details for PubMedID 39400761

    View details for PubMedCentralID 2997775

  • Results from A Comparative Study to Evaluate the Treatment Effectiveness of a Non-Pneumatic Compression Device versus an Advanced Pneumatic Compression Device for Lower Extremity Lymphedema Swelling (TEAYS study). Journal of vascular surgery. Venous and lymphatic disorders Barfield, M., Winokur, R., Berland, T., Davis, S., Ralph, V., Chatham, N., Rockson, S., Maldonado, T. S. 2024: 101965

    Abstract

    Advanced pneumatic compression devices (APCDs) have been shown to be effective in treatment of lower extremity lymphedema in the home setting. However, adherence to self-care has been poor, and APCD's require patients to remain immobile during treatment. We evaluated the safety and efficacy of a novel non-pneumatic compression device (NPCD) for treating lower extremity lymphedema vs and APCD.A randomized, crossover head-to-head study was performed at nine sites in 2023. Patients were randomized to either the NPCD or a commercially available APCD. Patients used the randomly assigned initial device for 28 days with a 4-week washout period before a comparable 28-day use of the second device.A total of 71 patients (108 affected limbs) with lower extremity lymphedema were analyzed. Compared with the APCD, the NPCD was associated with a greater mean reduction in limb edema volume (a mean limb volume reduction of 369.9 (± 68.19) mL p<0.05 vs 83.1 (± 67.99 mL) p<0.05). Significant improvement in Quality of Life was achieved for NPCD and but not for APCD treatment (score improvement of 1.01 (± 0.23) (p<0.05) for NPCD vs 0.17 (± 0.18) (p>0.05) for APCD). Patients reported greater adherence (81% vs 56%, p<0.001) and satisfaction with the NPCD (78% vs 22%) compared to APCD. No device related adverse events were reported.The novel NPCD is an effective treatment for reducing limb volume in patients with lower extremity lymphedema. The NPCD was more effective than an APCD and resulted in superior limb volume reduction, greater improved QoL, adherence, mobility, and patient satisfaction.

    View details for DOI 10.1016/j.jvsv.2024.101965

    View details for PubMedID 39222789

  • Focus on Lipedema: Unraveling the Mysteries Through Research. Lymphatic research and biology Rockson, S. G. 2024; 22 (2): 91-92

    View details for DOI 10.1089/lrb.2024.29161.editorial

    View details for PubMedID 38630992

  • The Role of Inflammation in Lymphedema: A Narrative Review of Pathogenesis and Opportunities for Therapeutic Intervention. International journal of molecular sciences Bowman, C., Rockson, S. G. 2024; 25 (7)

    Abstract

    Lymphedema is a chronic and progressive disease of the lymphatic system characterized by inflammation, increased adipose deposition, and tissue fibrosis. Despite early hypotheses identifying lymphedema as a disease of mechanical lymphatic disruption alone, the progressive inflammatory nature underlying this condition is now well-established. In this review, we provide an overview of the various inflammatory mechanisms that characterize lymphedema development and progression. These mechanisms contribute to the acute and chronic phases of lymphedema, which manifest clinically as inflammation, fibrosis, and adiposity. Furthermore, we highlight the interplay between current therapeutic modalities and the underlying inflammatory microenvironment, as well as opportunities for future therapeutic development.

    View details for DOI 10.3390/ijms25073907

    View details for PubMedID 38612716

  • Proposed Framework for Research Case Definitions of Lipedema. Lymphatic research and biology Keith, L., Seo, C., Wahi, M. M., Huggins, S., Carmody, M., Faerber, G., Forner-Cordero, I., Michelini, S., Rapprich, S., Rockson, S. G. 2024

    Abstract

    Background: Our aim is to propose a framework for the development of a research case definition of lipedema, based on current available literature and those observations that can be applied to future lipedema research with the intent to standardize and strengthen the scientific evidence base. Methods and Results: We conducted a narrative review of the literature, and identified consensus characteristics and disputed characteristics that could be included in a research case definition of lipedema. After considering the strength of the evidence and how each characteristic might be measured in a research study, we recommended an approach for the development of a research case definition of lipedema that would be based on consideration of five agreed-upon characteristics, and five disputed, or less substantiated, characteristics as additional evidence to enhance specificity. Conclusions: We present a case definition framework for lipedema drawn from the scientific literature that can be applied to future studies on lipedema. Utilizing this framework should help to increase the sensitivity and specificity of case definition and provide an opportunity for meta-analysis of clinical studies and facilitate future research intercomparisons.

    View details for DOI 10.1089/lrb.2023.0062

    View details for PubMedID 38546398

  • Genetic causes of lymphatic disorders: recent updates on the clinical and molecular aspects of lymphatic disease. Current opinion in cardiology Bowman, C., Rockson, S. G. 2024

    Abstract

    PURPOSE OF REVIEW: The lymphatic system facilitates several key functions that limit significant morbidity and mortality. Despite the impact and burden of lymphatic disorders, there are many remaining disorders whose genetic substrate remains unknown. The purpose of this review is to provide an update on the genetic causes of lymphatic disorders, while reporting on newly proposed clinical classifications of lymphatic disease.RECENT FINDINGS: We reviewed several new mutations in genes that have been identified as potential causes of lymphatic disorders including: MDFIC, EPHB4, and ANGPT2. Furthermore, the traditional St. George's Classification system for primary lymphatic anomalies has been updated to reflect the use of genetic testing, both as a tool for the clinical identification of lymphatic disease and as a method through which new sub-classifications of lymphatic disorders have been established within this framework. Finally, we highlighted recent clinical studies that have explored the impact of therapies such as sirolimus, ketoprofen, and acebilustat on lymphatic disorders.SUMMARY: Despite a growing body of evidence, current literature demonstrates a persistent gap in the number of known genes responsible for lymphatic disease entities. Recent clinical classification tools have been introduced in order to integrate traditional symptom- and time-based diagnostic approaches with modern genetic classifications, as highlighted in the updated St. George's classification system. With the introduction of this novel approach, clinicians may be better equipped to recognize established disease and, potentially, to identify novel causal mutations. Further research is needed to identify additional genetic causes of disease and to optimize current clinical tools for diagnosis and treatment.

    View details for DOI 10.1097/HCO.0000000000001116

    View details for PubMedID 38483006

  • Various Therapies for Lymphedema and Chronic Venous Insufficiency, Including a Multimodal At-Home Nonpneumatic Compression Treatment. Advances in skin & wound care Barnhart, H., Maldonado, T., Rockson, S. G. 2024

    Abstract

    Lymphedema and chronic venous insufficiency (CVI) affect millions of people and require lifelong management. Many compression options exist for the long-term management of these conditions; however, limitations in patient mobility and adherence are common. Current options for care often present challenges with adherence because they are time-intensive and cumbersome. Innovation is needed to improve compression options for patients with chronic edematous conditions, particularly because lymphedema and CVI benefit from combination interventions. In this narrative review, the authors focus on long-term management strategies for lymphedema and CVI and highlight a nonpneumatic compression device designed for ease of use in the management of lymphedema and CVI. Using a nonpneumatic compression device that combines multiple treatment modalities demonstrates improved efficacy, quality of life, and patient adherence.

    View details for DOI 10.1097/ASW.0000000000000091

    View details for PubMedID 38353650

  • Lipedema: Focus on Disease Magnitude and Quality-of-Life. Lymphatic research and biology Rockson, S. G. 2024; 22 (1): 1

    View details for DOI 10.1089/lrb.2024.29158.editorial

    View details for PubMedID 38394088

  • The Epigenetics of Lymphedema. Lymphatic research and biology Rockson, S. G. 2023; 21 (6): 535

    View details for DOI 10.1089/lrb.2023.29155.editorial

    View details for PubMedID 38149918

  • A quantitative analysis of lymphedema patient perceptions and subjective outcomes within the healthcare system Bowman, C., Rockson, S. G. SAGE PUBLICATIONS LTD. 2023: 500
  • Three-Dimensional Ultrasonography for Lipedema Diagnosis. Lymphatic research and biology Rockson, S. G. 2023; 21 (5): 431

    View details for DOI 10.1089/lrb.2023.29151.editorial

    View details for PubMedID 37870782

  • Effectiveness of a Nonpneumatic Active Compression Device in Older Adults with Breast Cancer-Related Lymphedema: A Subanalysis of a Randomized Crossover Trial. Lymphatic research and biology Rockson, S. G., Skoracki, R. 2023

    Abstract

    Background: A recently completed clinical trial compared a novel nonpneumatic compression device (NPCD) with a traditional advanced pneumatic compression device (APCD) for the treatment of breast cancer-related lymphedema (BCRL); the study revealed that the NPCD produced superior clinical and quality-of-life (QOL) outcomes. In this subanalysis, we sought to examine these results within the subset of trial subjects aged ≥65 years. Methods: A randomized crossover head-to-head trial was conducted to compare the NPCD with a commercially available APCD. Patients were randomly assigned to one or the other device for 28 days of use, followed by a 4-week washout period before a comparable 28-day utilization of the alternate device. Limb edema, adherence to daily device use, and QOL measures were collected at day 0 and 28 of each period. Results: A total of 14 subjects were aged ≥65. During NPCD use, subjects experienced a mean decrease in limb edema of 100.3% (p = 0.0082) as well as improvements in mean overall and subscale scores of the Lymphedema Quality of Life Questionnaire (LYMQOL). By comparison, during APCD use limb edema decreased by a mean of 2.9% (p = 0.8899) with no significant changes in any LYMQOL scores. Mean adherence was significantly higher during NPCD use (96.6%) than during APCD use (58.3%, p < 0.0001). Conclusions: The novel NPCD produced superior clinical and QOL outcomes in older subjects with BCRL. ClinicalTrials.gov ID: NCT04908254.

    View details for DOI 10.1089/lrb.2022.0085

    View details for PubMedID 37729078

  • Lymphatic Malformations: What Can We Learn from the Fluid. Lymphatic research and biology Rockson, S. G. 2023; 21 (4): 338

    View details for DOI 10.1089/lrb.2023.29147.editorial

    View details for PubMedID 37616584

  • Lymphedema self-care: economic cost savings and opportunities to improve adherence. Cost effectiveness and resource allocation : C/E Karaca-Mandic, P., Solid, C. A., Armer, J. M., Skoracki, R., Campione, E., Rockson, S. G. 2023; 21 (1): 47

    Abstract

    BACKGROUND: Breast cancer-related lymphedema (BCRL) imposes a significant economic burden on patients, providers, and society. There is no curative therapy for BCRL, but management through self-care can reduce symptoms and lower the risk of adverse events.MAIN BODY: The economic burden of BCRL stems from related adverse events, reductions in productivity and employment, and the burden placed on non-medical caregivers. Self-care regimens often include manual lymphatic drainage, compression garments, and meticulous skin care, and may incorporate pneumatic compression devices. These regimens can be effective in managing BCRL, but patients cite inconvenience and interference with daily activities as potential barriers to self-care adherence. As a result, adherence is generally poor and often worsens with time. Because self-care is on-going, poor adherence reduces the effectiveness of regimens and leads to costly treatment of BCRL complications.CONCLUSION: Novel self-care solutions that are more convenient and that interfere less with daily activities could increase self-care adherence and ultimately reduce complication-related costs of BCRL.

    View details for DOI 10.1186/s12962-023-00455-7

    View details for PubMedID 37516870

  • Development of a rat model of lymphedema and the implantation of a collagen-based medical device for therapeutic intervention. Frontiers in cardiovascular medicine Nguyen, D., Dionyssiou, D., Zaitseva, T. S., Zhou, A. T., Sue, G., Deptula, P., Moroz, M. A., Tabada, P., Rockson, S. G., Paukshto, M. V., Cheng, M. H., Huang, N. F. 2023; 10: 1214116

    Abstract

    Secondary lymphedema is a common condition among cancer survivors, and treatment strategies to prevent or treat lymphedema are in high demand. The development of novel strategies to diagnose or treat lymphedema would benefit from a robust experimental animal model of secondary lymphedema. The purpose of this methods paper is to describe and summarize our experience in developing and characterizing a rat hindlimb model of lymphedema. Here we describe a protocol to induce secondary lymphedema that takes advantage of micro computed tomography imaging for limb volume measurements and visualization of lymph drainage with near infrared imaging. To demonstrate the utility of this preclinical model for studying the therapeutic benefit of novel devices, we apply this animal model to test the efficacy of a biomaterials-based implantable medical device.

    View details for DOI 10.3389/fcvm.2023.1214116

    View details for PubMedID 37469481

    View details for PubMedCentralID PMC10353614

  • Abnormal lymphatic S1P signaling aggravates lymphatic dysfunction and tissue inflammation. medRxiv : the preprint server for health sciences Kim, D., Tian, W., Wu, T. T., Xiang, M., Vinh, R., Chang, J., Gu, S., Lee, S., Zhu, Y., Guan, T., Schneider, E. C., Bao, E., Dixon, J. B., Kao, P., Pan, J., Rockson, S. G., Jiang, X., Nicolls, M. R. 2023

    Abstract

    BACKGROUND: Lymphedema is a global health problem with no effective drug treatment. Enhanced T cell immunity and abnormal lymphatic endothelial cell (LEC) signaling are promising therapeutic targets for this condition. Sphingosine-1-phosphate (S1P) mediates a key signaling pathway required for normal LEC function, and altered S1P signaling in LECs could lead to lymphatic disease and pathogenic T cell activation. Characterizing this biology is relevant for developing much-needed therapies.METHODS: Human and mouse lymphedema was studied. Lymphedema was induced in mice by surgically ligating the tail lymphatics. Lymphedematous dermal tissue was assessed for S1P signaling. To verify the role of altered S1P signaling effects in lymphatic cells, LEC-specific S1pr1 -deficient ( S1pr1 LECKO ) mice were generated. Disease progression was quantified by tail-volumetric and -histopathological measurements over time. LECs from mice and humans, with S1P signaling inhibition, were then co-cultured with CD4 T cells, followed by an analysis of CD4 T cell activation and pathway signaling. Finally, animals were treated with a monoclonal antibody specific to P-selectin to assess its efficacy in reducing lymphedema and T cell activation.RESULTS: Human and experimental lymphedema tissues exhibited decreased LEC S1P signaling through S1PR1. LEC S1pr1 loss-of-function exacerbated lymphatic vascular insufficiency, tail swelling, and increased CD4 T cell infiltration in mouse lymphedema. LECs, isolated from S1pr1 LECKO mice and co-cultured with CD4 T cells, resulted in augmented lymphocyte differentiation. Inhibiting S1PR1 signaling in human dermal LECs (HDLECs) promoted T helper type 1 and 2 (Th1 and Th2) cell differentiation through direct cell contact with lymphocytes. HDLECs with dampened S1P signaling exhibited enhanced P-selectin, an important cell adhesion molecule expressed on activated vascular cells. In vitro , P-selectin blockade reduced the activation and differentiation of Th cells co-cultured with sh S1PR1 -treated HDLECs. P-selectin-directed antibody treatment improved tail swelling and reduced Th1/Th2 immune responses in mouse lymphedema.CONCLUSION: This study suggests that reduction of the LEC S1P signaling aggravates lymphedema by enhancing LEC adhesion and amplifying pathogenic CD4 T cell responses. P-selectin inhibitors are suggested as a possible treatment for this pervasive condition.Clinical Perspective: What is New?: Lymphatic-specific S1pr1 deletion exacerbates lymphatic vessel malfunction and Th1/Th2 immune responses during lymphedema pathogenesis. S1pr1 -deficient LECs directly induce Th1/Th2 cell differentiation and decrease anti-inflammatory Treg populations. Peripheral dermal LECs affect CD4 T cell immune responses through direct cell contact.LEC P-selectin, regulated by S1PR1 signaling, affects CD4 T cell activation and differentiation.P-selectin blockade improves lymphedema tail swelling and decreases Th1/Th2 population in the diseased skin.What Are the Clinical Implications?: S1P/S1PR1 signaling in LECs regulates inflammation in lymphedema tissue.S1PR1 expression levels on LECs may be a useful biomarker for assessing predisposition to lymphatic disease, such as at-risk women undergoing mastectomyP-selectin Inhibitors may be effective for certain forms of lymphedema.

    View details for DOI 10.1101/2023.06.08.23291175

    View details for PubMedID 37398237

  • Lymphatics in Space. Lymphatic research and biology Rockson, S. G. 2023; 21 (3): 229

    View details for DOI 10.1089/lrb.2023.29144.editorial

    View details for PubMedID 37358830

  • Treatment of rat lymphedema by propeller lymphatic tissue flap combined with nano-fibrillar collagen scaffolds. Journal of reconstructive microsurgery Dionyssiou, D., Nguyen, D., Topalis, A., Deptula, P., Paukshto, M., Zaitseva, T., Demiri, E., Cheva, A., Rockson, S. 2023

    Abstract

    Background The aim of our study was to evaluate a new propeller vascularized lymphatic tissue flap (pLNT) combined with aligned nanofibrillar collagen scaffolds (CS) (BioBridge®) in reducing lymphedema in the rat lymphedema model. Methods Unilateral left hind limb lymphedema was created in 15 female Sprague-Dawley rats following inguinal and popliteal lymph nodes (LN) resection and radiation. An inguinal pLNT was elevated from the contralateral groin and transferred through a skin tunnel to the affected groin. Four collagen threads were attached to the flap and inserted in the hind limb at the subcutaneous level in a fan shape. The three study groups consisted of Group A (control), Group B (pLNT), and Group C (pLNT + CS). Volumetric analysis of both hind limbs was performed using micro-CT imaging before the surgery (at initial time point) and then at 1 and 4 months postoperatively, and the relative volume difference (excess volume) was measured for each animal. Lymphatic drainage was assessed by ICG fluoroscopy for number and morphology of new collectors and the time required for ICG to move from injection point to the midline. Results Four months after the surgery an increased relative volume difference remained in group A (5,321% ± 4,74), while there was a significant relative volume reduction in group B (-13,395% ± 8,545) and an even greater reduction in group C (-14,560% ± 5,042). ICG fluoroscopy proved the functional restoration of lymphatic vessels through the CS and the viability of pLNT in both B and C groups. Conclusion The pedicle lymphatic tissue flap combined with collagen scaffolds is an effective procedure for the treatment of lymphedema in rats. It can be easily translated into treatment of humans' lower and upper limb lymphedema; further clinical studies are required prior to recommend the above method.

    View details for DOI 10.1055/a-2086-0269

    View details for PubMedID 37142251

  • Acupuncture Treatment for Breast Cancer-Related Lymphedema: A Randomized Pilot Study. Lymphatic research and biology Friedman, R., Johnson, A. R., Shillue, K., Fleishman, A., Mistretta, C., Magrini, L., Tran, B. N., Rockson, S. G., Lu, W., Yeh, G. Y., Singhal, D. 2023

    Abstract

    Background: Methods of conservative management for breast cancer-related lymphedema (BCRL) are burdensome in terms of time, cost, and convenience. In addition, many patients are not candidates for surgical treatment. Preliminary results have demonstrated possible beneficial effects of acupuncture for patients with BCRL. In this small pilot study, we examined the safety and feasibility of an acupuncture randomized control trial (RCT) in this patient cohort, utilizing a battery of standardized clinical and patient-centered outcome measures. Methods and Results: Patients with BCRL were randomized 2:1 to the acupuncture (n = 10) or the control (n = 4) group. Patients received acupuncture to the unaffected extremity biweekly for 6 weeks. Feasibility was defined as enrollment ≥80%, completion of ≥9 of 12 acupuncture sessions per person, and ≥75% completion of three of three measurement visits. To inform a future adequately powered RCT, we describe within-group changes in patient-centered outcomes, including circumferential measurements, bioimpedance spectroscopy, perometry, cytokine levels, and patient quality of life. Adverse events were systematically tracked. Fourteen patients completed the study. Of those who received acupuncture (n = 10), 8 completed all 12 acupuncture sessions, and 2 patients completed 11 sessions. Ninety-three percent of all participants completed all three measurement visits. There was no consistent improvement in arm volumes. Inflammatory marker levels had inconclusive fluctuations among both groups. All patients receiving acupuncture demonstrated an improvement in their functional quality-of-life score. No severe adverse events occurred. Conclusions: A randomized controlled study of acupuncture for BCRL is feasible. The acupuncture intervention is acceptable in this population, without safety concerns in a small sample and warrants further investigation.

    View details for DOI 10.1089/lrb.2022.0001

    View details for PubMedID 37083501

  • Breast Cancer-Related Lymphedema: The Primary/Secondary Conundrum. Lymphatic research and biology Rockson, S. G. 2023; 21 (2): 99-100

    View details for DOI 10.1089/lrb.2023.29141.editorial

    View details for PubMedID 37093173

  • Final Analysis (NILE): A Randomized Control Cross-Over Clinical Study Comparing Dayspring: A Novel Wearable Compression Technology to Pneumatic Compression Device in the Treatment of Lymphedema Rockson, S. G., Skoracki, R., Armer, J. MOSBY-ELSEVIER. 2023: 45S
  • Fake-news-free evidence-based communication for proper vein-lymphatic disease management. International angiology : a journal of the International Union of Angiology Gianesini, S., Chi, Y. W., Agüero, C., Alqedrah, D., Amore, M., Barbati, M., Baturone, A., Black, S., Borsuk, D., Bottini, O., Caprini, J., Chamo, M., Cherian, M., Chernuka, L., DE Maeseneer, M., Diaz, J., Garcia, M. J., Gibson, K., Gloviczki, M., Gloviczki, P., Golovina, V., Goranova, E., Grillo, L., Gwozdz, A., Hirsch, T., Hussein, E., Intriago, E., Jalaie, H., Jaworucka-Kaczorowska, A., Jindal, R., Josnin, M., Khilnani, N. M., Kim, D. I., Latorre, A., Lazarashvili, Z., Lee, B. B., Leon, L., Liew, N. C., Lobastov, K., Lurie, F., Maghetti, A., Menegatti, E., Miyake, K., Mo, M., Narayanan, S., Neuhardt, D., Pannier, F., Prego, A., Rabe, E., Raffetto, J., Raymond-Martimbeau, P., Redman, L., Reina-Gutierrez, L., Rial, R., Rockson, S., Romanelli, M., Santiago, F. R., Santiago, R. A., Sermsathanasawadi, N., Shaydakov, E., Simkin, C., Sousa, J., Stoughton, J., Szuba, A., Taha, W., Ulloa, J., Urbanek, T., Vitale, M., Vuylsteke, M., Wang, J., Weingartner, J., Wilson, S., Yamaki, T., Ng, Y., Zolotukhin, I., Mansilha, A. 2023

    Abstract

    Published scientific evidence demonstrate the current spread of healthcare misinformation in the most popular social networks and unofficial communication channels. Up to 40% of the medical websites were identified reporting inappropriate information, moreover being shared more than 450,000 times in a 5-year-time frame. The phenomenon is particularly spread in infective diseases medicine, oncology and cardiovascular medicine. The present document is the result of a scientific and educational endeavor by a worldwide group of top experts who selected and analyzed the major issues and related evidence-based facts on vein and lymphatic management. A section of this work is entirely dedicated to the patients and therefore written in layman terms, with the aim of improving public vein-lymphatic awareness. The part dedicated to the medical professionals includes a revision of the current literature, summing up the statements that are fully evidence-based in venous and lymphatic disease management, and suggesting future lines of research to fulfill the still unmet needs. The document has been written following an intense digital interaction among dedicated working groups, leading to an institutional project presentation during the Universal Expo in Dubai, in the occasion of the v-WINter 2022 meeting.

    View details for DOI 10.23736/S0392-9590.23.05044-7

    View details for PubMedID 36930179

  • Lymphedema: A Symphony of Fat and Scar. Lymphatic research and biology Rockson, S. G. 2023; 21 (1): 1

    View details for DOI 10.1089/lrb.2023.29138.editorial

    View details for PubMedID 36809170

  • Author Correction: A non-randomized, open-label study of the safety and effectiveness of a novel non-pneumatic compression device (NPCD) for lower limb lymphedema. Scientific reports Rockson, S. G., Karaca-Mandic, P., Nguyen, M., Shadduck, K., Gingerich, P., Campione, E., Hetrrick, H. 2023; 13 (1): 911

    View details for DOI 10.1038/s41598-023-28027-y

    View details for PubMedID 36650179

  • Cancer-Related Lymphedema: Primary or Secondary? Lymphatic research and biology Rockson, S. G. 2022; 20 (6): 579

    View details for DOI 10.1089/lrb.2022.29134.editorial

    View details for PubMedID 36537707

  • A Novel Genetic Candidate for Primary Lymphedema. Lymphatic research and biology Rockson, S. G. 2022; 20 (5): 467

    View details for DOI 10.1089/lrb.2022.29131.editorial

    View details for PubMedID 36302177

  • A non-randomized, open-label study of the safety and effectiveness of a novel non-pneumatic compression device (NPCD) for lower limb lymphedema. Scientific reports Rockson, S. G., Karaca-Mandic, P., Nguyen, M., Shadduck, K., Gingerich, P., Campione, E., Hetrrick, H. 2022; 12 (1): 14005

    Abstract

    Lower extremity lymphedema (LEL) can result in detriments to quality of life (QOL) and impose a significant economic burden on patients and payers. A common component of treatment is pneumatic compression, which requires patients toremain immobile. We investigated a novel non-pneumatic compression device (NPCD) that allows patients to remain active during compression treatment, to see if it reduces swelling and improves QOL. We conducted a non-randomized, open-label, 12-week pilot study of adult patients with primary or secondary unilateral LEL, and measured changes in limb edema and QOL using the Lymphedema Quality of Life Questionnaire (LYMQOL). Twenty-four subjects were enrolled; the majority were female (17) with secondary lymphedema (21). Eighteen completed the study. Statistically significant improvements were observed in overall QOL, aggregated LYMQOL total score, and three of four LYMQOL subscales (Function, Appearance, Mood). The fourth (Symptoms) trended toward significant improvement (p=0.06). The average reduction in affected limb edema was 39.4%. The novel NPCD produced statistically significant improvements in QOL, functioning, and edema volume of patients with LEL. Innovations in devices to manage LEL can be effective while allowing patients to maintain mobility and physical activity during treatment.

    View details for DOI 10.1038/s41598-022-17225-9

    View details for PubMedID 35977981

  • Safety and Effectiveness of a Novel Non-Pneumatic Active Compression Device for Treating Breast Cancer-Related Lymphedema, a Multi-center Randomized, Crossover Trial (NILE). Journal of vascular surgery. Venous and lymphatic disorders Rockson, S. G., Whitworth, P. W., Cooper, A., Kania, S., Karnofel, H., Nguyen, M., Shadduck, K., Gingerich, P., Armer, J. 2022

    Abstract

    Advanced pneumatic compression devices (APCDs) have been shown to be an effective intervention for lymphedema when used as part of a self-care maintenance treatment regimen. However, adherence to self-care is poor, and APCDs require patients to be immobile during treatment. We sought to evaluate the safety and efficacy of a novel non-pneumatic compression device (NPCD) for treating lymphedema versus an APCD.A randomized, crossover head-to-head investigation at five US sites in 2021. Patients were randomized to either the NPCD or a commercially-available APCD. Subjects used the randomly assigned initial device for 28 days with a 4-week washout period prior to a comparable 28-day utilization of the second device.Data from 50 adult women with unilateral breast cancer-related lymphedema (BCRL) were analyzed. When compared with the APCD, the NPCD was associated with greater mean reduction in limb edema volume (64.6% vs. 27.7%, p<0.001), significantly greater mean improvements in quality of life scores, greater adherence (95.6% vs. 49.8%, p<0.001), and greater satisfaction with the device (90% vs. 14%, p<0.001). Patients indicated that the NPCD facilitated exercise and was convenient for travel. No adverse events were reported.The novel NPCD is an effective maintenance treatment for reducing limb volume in BCRL patients. The device was more effective than an APCD and resulted in higher adherence to self-care interventions and greater patient satisfaction.

    View details for DOI 10.1016/j.jvsv.2022.06.016

    View details for PubMedID 35952956

  • The Impact of Dietary Fat in Lymphatic Anomalies. Lymphatic research and biology Rockson, S. G. 2022; 20 (4): 357

    View details for DOI 10.1089/lrb.2022.29128.editorial

    View details for PubMedID 35993924

  • Early Investigation of the Gut-Lymph Concept. Lymphatic research and biology Rockson, S. G. 2022; 20 (3): 247

    View details for DOI 10.1089/lrb.2022.29125.sr

    View details for PubMedID 35687829

  • Management of Complex Lymphatic Anomalies with Severe Bony Involvement. Lymphatic research and biology Rockson, S. G. 2022; 20 (2): 117

    View details for DOI 10.1089/lrb.2022.29122.sr

    View details for PubMedID 35467971

  • The American venous forum, American vein and lymphatic society and the society for vascular medicine expert opinion consensus on lymphedema diagnosis and treatment. Phlebology Lurie, F., Malgor, R. D., Carman, T., Dean, S. M., Iafrati, M. D., Khilnani, N. M., Labropoulos, N., Maldonado, T. S., Mortimer, P., O'Donnell, T. F., Raffetto, J. D., Rockson, S. G., Gasparis, A. P. 2022: 2683555211053532

    Abstract

    BACKGROUND: Lymphedema imposes a significant economic and social burden in modern societies. Controversies about its risk factors, diagnosis, and treatment permeate the literature. The goal of this study was to assess experts' opinions on the available literature on lymphedema while following the Delphi methodology.METHODS: In December of 2019, the American Venous Forum created a working group tasked to develop a consensus statement regarding current practices for the diagnosis and treatment of lymphedema. A panel of experts was identified by the working group. The working group then compiled a list of clinical questions, risk factors, diagnosis and evaluation, and treatment of lymphedema. Fifteen questions that met the criteria for consensus were included in the list. Using a modified Delphi methodology, six questions that received between 60% and 80% of the votes were included in the list for the second round of analysis. Consensus was reached whenever >70% agreement was achieved.RESULTS: The panel of experts reached consensus that cancer, infection, chronic venous disease, and surgery are risk factors for secondary lymphedema. Consensus was also reached that clinical examination is adequate for diagnosing lymphedema and that all patients with chronic venous insufficiency (C3-C6) should be treated as lymphedema patients. No consensus was reached regarding routine clinical practice use of radionuclide lymphoscintigraphy as a mandatory diagnostic tool. However, the panel came to consensus regarding the importance of quantifying edema in all patients (93.6% in favor). In terms of treatment, consensus was reached favoring the regular use of compression garments to reduce lymphedema progression (89.4% in favor, 10.6% against; mean score of 79), but the use of Velcro devices as the first line of compression therapy did not reach consensus (59.6% in favor vs 40.4% against; total score of 15). There was agreement that sequential pneumatic compression should be considered as adjuvant therapy in the maintenance phase of treatment (91.5% in favor vs. 8.5% against; mean score of 85), but less so in its initial phases (61.7% in favor vs. 38.3% against; mean score of 27). Most of the panel agreed that manual lymphatic drainage should be a mandatory treatment modality (70.2% in favor), but the panel was split in half regarding the proposal that reductive surgery should be considered for patients with failed conservative treatment.CONCLUSION: This consensus process demonstrated that lymphedema experts agree on the majority of the statements related to risk factors for lymphedema, and the diagnostic workup for lymphedema patients. Less agreement was demonstrated on statements related to treatment of lymphedema. This consensus suggests that variability in lymphedema care is high even among the experts. This information should be considered by developers of future practice guidelines for lymphedema, especially in cases of low-level evidence that supports practice patterns with which the majority of experts disagree.

    View details for DOI 10.1177/02683555211053532

    View details for PubMedID 35258350

  • Objective Noninvasive Detection and Documentation of Upper and Lower Extremity Lymphedema. Lymphatic research and biology Rockson, S. G. 2022; 20 (1): 1-2

    View details for DOI 10.1089/lrb.2022.29120.sr

    View details for PubMedID 35226536

  • Hypoxia and Hypoxia-Inducible Factors in Lymphedema. Frontiers in pharmacology Jiang, X., Tian, W., Kim, D., McQuiston, A. S., Vinh, R., Rockson, S. G., Semenza, G. L., Nicolls, M. R. 2022; 13: 851057

    Abstract

    Lymphedema is a chronic inflammatory disorder characterized by edema, fat deposition, and fibrotic tissue remodeling. Despite significant advances in lymphatic biology research, our knowledge of lymphedema pathology is incomplete. Currently, there is no approved pharmacological therapy for this debilitating disease. Hypoxia is a recognized feature of inflammation, obesity, and fibrosis. Understanding hypoxia-regulated pathways in lymphedema may provide new insights into the pathobiology of this chronic disorder and help develop new medicinal treatments.

    View details for DOI 10.3389/fphar.2022.851057

    View details for PubMedID 35450048

  • Extending Diagnostic Imaging Accuracy in Lymphedema. Lymphatic research and biology Rockson, S. G. 1800; 19 (6): 515-516

    View details for DOI 10.1089/lrb.2021.29115.sr

    View details for PubMedID 34958251

  • Clinical Evaluation of a Novel Wearable Compression Technology in the Treatment of Lymphedema, an Open-Label Controlled Study. Lymphatic research and biology Rockson, S. G., Karaca-Mandic, P., Skoracki, R., Hock, K., Nguyen, M., Shadduck, K., Gingerich, P., Campione, E., Leifer, A., Armer, J. 2021

    Abstract

    A diagnosis of lymphedema comes with a lifetime requirement for careful self-care and treatment to control skin deterioration and the consequences of excessive fluid and protein buildup leading to abnormal limb volume and an increased risk of infection. The burden of care and psychosocial aspects of physical disfiguration and loss of function are associated with compromised quality of life (QoL). The current standard therapeutic intervention is complex decongestive therapy with manual lymph drainage and frequent wearing of compression garments. With insurance limitations on therapy visits and the time and travel required, additional home treatment options are needed. Pneumatic compression pumps that mimic the manual massage pressure and pattern are sometimes prescribed, but these are bulky, difficult to apply, and require immobility during treatment. An open-label pilot study in 40 subjects was performed to evaluate the QoL and limb volume maintenance efficacy of a novel wearable compression system (Dayspring) that is low profile, easy to use, and allows for mobility during treatment. After 28 days of use, subjects had a statistically significant 18% (p<0.001) improvement in overall QoL as measured by the Lymphedema Quality-of-Life Questionnaire compared with baseline. Individual QoL domains, and limb volume improved with therapy. Adherence was 98% over the course of the study. Results of the clinical evaluation suggest the Dayspring wearable compression device is safe and effective and improves QoL and limb volume. The novel, low-profile device is easy to use and allows for mobility during treatment, addressing a potential barrier to adherence with pneumatic compression devices.

    View details for DOI 10.1089/lrb.2020.0126

    View details for PubMedID 34227842

  • Lymphatic Endothelial Barrier Integrity and the Sigma-1 Receptor. Lymphatic research and biology Rockson, S. G. 2021; 19 (3): 205

    View details for DOI 10.1089/lrb.2021.29105.sr

    View details for PubMedID 34137648

  • The Kinetics of Lymphatic Dysfunction and Leukocyte Expansion in the Draining Lymph Node during LTB4 Antagonism in a Mouse Model of Lymphedema. International journal of molecular sciences Cribb, M. T., Sestito, L. F., Rockson, S. G., Nicolls, M. R., Thomas, S. N., Dixon, J. B. 2021; 22 (9)

    Abstract

    The mechanisms of lymphedema development are not well understood, but emerging evidence highlights the crucial role the immune system plays in driving its progression. It is well known that lymphatic function deteriorates as lymphedema progresses; however, the connection between this progressive loss of function and the immune-driven changes that characterize the disease has not been well established. In this study, we assess changes in leukocyte populations in lymph nodes within the lymphatic drainage basin of the tissue injury site (draining lymph nodes, dLNs) using a mouse tail model of lymphedema in which a pair of draining collecting vessels are left intact. We additionally quantify lymphatic pump function using established near infrared (NIR) lymphatic imaging methods and lymph-draining nanoparticles (NPs) synthesized and employed by our team for lymphatic tissue drug delivery applications to measure lymphatic transport to and resulting NP accumulation within dLNs associated with swelling following surgery. When applied to assess the effects of the anti-inflammatory drug bestatin, which has been previously shown to be a possible treatment for lymphedema, we find lymph-draining NP accumulation within dLNs and lymphatic function to increase as lymphedema progresses, but no significant effect on leukocyte populations in dLNs or tail swelling. These results suggest that ameliorating this loss of lymphatic function is not sufficient to reverse swelling in this surgically induced disease model that better recapitulates the extent of lymphatic injury seen in human lymphedema. It also suggests that loss of lymphatic function during lymphedema may be driven by immune-mediated mechanisms coordinated in dLNs. Our work indicates that addressing both lymphatic vessel dysfunction and immune cell expansion within dLNs may be required to prevent or reverse lymphedema when partial lymphatic function is sustained.

    View details for DOI 10.3390/ijms22094455

    View details for PubMedID 33923272

  • Lymphedema, Inflammation, and Fat. Lymphatic research and biology Rockson, S. G. 2021; 19 (2): 115

    View details for DOI 10.1089/lrb.2021.29103.sr

    View details for PubMedID 33900825

  • Research Priorities in Lymphatic Interventions: Recommendations from a Multidisciplinary Research Consensus Panel. Journal of vascular and interventional radiology : JVIR Itkin, M., Rockson, S. G., Witte, M. H., Burkhoff, D., Phillips, A., Windsor, J. A., Kassab, G. S., Hur, S., Nadolski, G., Pabon-Ramos, W. M., Rabinowitz, D., White, S. B. 2021

    Abstract

    Recognizing the increasing importance of lymphatic interventions, the Society of Interventional Radiology Foundation brought together a multidisciplinary group of key opinion leaders in lymphatic medicine to define the priorities in lymphatic research. On February 21, 2020, SIRF convened a multidisciplinary Research Consensus Panel (RCP) of experts in the lymphatic field. During the meeting, the panel and audience discussed potential future research priorities. The panelists ranked the discussed research priorities based on clinical relevance, overall impact, and technical feasibility. The following research topics were prioritized by RCP: lymphatic decompression in patients with congestive heart failure, detoxification of thoracic duct lymph in acute illness, development of newer agents for lymphatic imaging, characterization of organ-based lymph composition, and development of lymphatic interventions to treat ascites in liver cirrhosis. The RCP priorities underscored that the lymphatic system plays an important role not only in the intrinsic lymphatic diseases but in conditions that traditionally are not considered to be lymphatic such as congestive heart failure, liver cirrhosis, and critical illness. The advancement of the research in these areas will lead the field of lymphatic interventions to the next level.

    View details for DOI 10.1016/j.jvir.2021.01.269

    View details for PubMedID 33610432

  • Establishing Standards for Centers of Excellence for the Diagnosis and Treatment of Lymphatic Disease. Lymphatic research and biology Chang, D., Dayan, J., Fried, P., Patel, K., Repicci, W., Rockson, S., Singhal, D., Aldrich, M. B. 2021

    Abstract

    Background: Lymphatic disease patients make up a significant proportion of the US and world populations. Due to inadequate medical school training and underestimation of the impact of lymphatic circulation, lymphatic disease patients often have difficulty finding competent diagnosis and care. Methods and Results: The Lymphatic Education & Research Network has initiated a Centers of Excellence program to designate institutions that provide services for lymphatic disease patients. Committees of experts drafted standards for five types of Centers of Excellence. Conclusions: The Centers of Excellence program is now launched, and the description of the formation process herein could provide other organizations guidance for similar ventures.

    View details for DOI 10.1089/lrb.2020.0022

    View details for PubMedID 33544022

  • Lymphatic Development and Implications for Diagnosis and Therapy. Lymphatic research and biology Desai, S. B., Iacobas, I. n., Rockson, S. G. 2021; 19 (1): 31–35

    Abstract

    The lymphatic system was first described in the 17th century independently by Olaus Rudbeck and Thomas Bartholin. Since then, there has been deep-seated fascination with its development, function, and dysfunction.

    View details for DOI 10.1089/lrb.2020.0123

    View details for PubMedID 33625891

  • Management of Lymphatic Vascular Malformations: A Systematic Review of the Literature. Journal of vascular surgery. Venous and lymphatic disorders Kalwani, N. M., Rockson, S. G. 2021

    Abstract

    Lymphatic malformations (LM) are common congenital vascular lesions, most often diagnosed at birth. They deform local anatomy and can be life-threatening if they compress the aerodigestive tract or other vital structures. Significant progress has been made in the treatment of LM in the past twenty years. We conducted a systematic review of the literature on the management of LM.On September 21, 2020, we searched PubMed/MEDLINE for studies published from 2000 to 2020 reporting outcomes of invasive and pharmacologic treatment of LM.A total of 251 studies met eligibility criteria. Surgery continues to be a mainstay in the management of LM, especially in the treatment of microcystic and mixed lesions. Sclerotherapy has emerged as a first-line treatment for macrocystic LM and as an adjunctive therapy used in combination with surgery for other lesions. Sirolimus, a strong inhibitor of mTOR, has shown tremendous promise in the treatment of LM, both as an oral and a topical agent. Recent investigations have shown the potential of targeted small molecule modulators of cellular pathways in the treatment of LM.Multiple invasive and pharmacologic therapies have been shown to be effective in the treatment of LM. Future research should focus on rigorous, prospective comparisons of these treatment modalities.

    View details for DOI 10.1016/j.jvsv.2021.01.013

    View details for PubMedID 33540133

  • Comorbidity and Lymphatic Disease: The Lymphatic Continuum Re-Examined. Lymphatic research and biology Rockson, S. G. 2021; 19 (1): 17–19

    Abstract

    It has now been ∼20 years since the original Lymphatic Continuum conference was convened, and this continuum has transitioned from a compelling concept to a reality. The explosive growth in our comprehension of lymphatic genetics, development, and function has expanded and modified our traditional views regarding what is, and is not, lymphatic disease. Groundbreaking investigations over the past decade have now defined a large and growing list of pathological conditions in which morphological or function lymphatic alterations can be identified. This list includes atherosclerosis and dyslipidemia, hypertension and other cardiovascular diseases, inflammation and inflammatory bowel disease, obesity, narrow angle glaucoma, and, most recently and compellingly, neurodegenerative disease. The sometimes overlapping but largely disparate nature of these various aforementioned disease categories suggests that the presence, or absence, of structural or functional lymphatic derangements may represent a previously unrecognized unifying influence in the maintenance of health and the promotion of disease. Future investigation of lymphatic mechanisms in disease will likely continue to elucidate the influences of lymphatic dysfunction, perhaps subtle, that can invest other, seemingly unrelated, diseases. In future, such discoveries will provide mechanistic insights and may potentiate the development of a new lymphatic-based approach to human disease diagnosis and therapeutics.

    View details for DOI 10.1089/lrb.2021.0001

    View details for PubMedID 33625889

  • Lymphatic Centers of Excellence: A New Reality, Long Overdue. Lymphatic research and biology Rockson, S. G. 2021; 19 (1): 1–2

    View details for DOI 10.1089/lrb.2021.29100.sr

    View details for PubMedID 33625890

  • Inhibition of Fibrosis to Combat Lymphedema. Lymphatic research and biology Rockson, S. G. 2020; 18 (5): 399

    View details for DOI 10.1089/lrb.2020.29093.sr

    View details for PubMedID 33107757

  • Leukotrienes in Tumor-Associated Inflammation FRONTIERS IN PHARMACOLOGY Tian, W., Jiang, X., Kim, D., Guan, T., Nicolls, M. R., Rockson, S. G. 2020; 11
  • The Beguiling Histopathology of the Axillary Web Syndrome. Lymphatic research and biology Rockson, S. G. 2020; 18 (4): 321

    View details for DOI 10.1089/lrb.2020.29090.sr

    View details for PubMedID 32822259

  • Bioimpedance Analysis of Lower Extremity Lymphedema. Lymphatic research and biology Rockson, S. G. 2020; 18 (2): 98

    View details for DOI 10.1089/lrb.2020.29085.sr

    View details for PubMedID 32320345

  • Feasibility and Reliability of Rapid Diagnosis of Myocardial Infarction AMERICAN JOURNAL OF THE MEDICAL SCIENCES Engel, G., Rockson, S. G. 2020; 359 (2): 73–78
  • Alzheimer's Disease: Can the Meningeal Lymphatics Provide the Answer? Lymphatic research and biology Rockson, S. G. 2020; 18 (1): 1

    View details for DOI 10.1089/lrb.2020.29078.sr

    View details for PubMedID 32077798

  • Feasibility and Reliability of Rapid Diagnosis of Myocardial Infarction. The American journal of the medical sciences Engel, G., Rockson, S. G. 2020; 359 (2): 73-78

    Abstract

    Prevailing hospital practice dictates a protracted phase of observation for patients with chest pain to establish or exclude the diagnosis of myocardial infarction. Early diagnosis of acute myocardial infarction may improve patient care and reduce both complications and hospital costs. A study was performed to investigate the feasibility of early diagnosis of myocardial infarction within the first 9 hours of the hospital stay.The records of all patients admitted with chest pain within one calendar year were analyzed. The timing of creatine kinase-MB (CK-MB) quantification was determined with reference to the initial phlebotomy (time 0). An enzymatic diagnosis of myocardial infarction was assigned if any determination of CK-MB exceeded the upper limit of normal, and the diagnosis of each patient at or before 9 hours (early diagnosis) was compared to the ultimate diagnosis at 14 to 24 hours (final diagnosis) beyond initial assessment.Of the 528 included patients, 523 patients (99.1%) had identical early and final diagnostic outcomes; 5 patients (0.9%) had conflicting results. An early diagnosis of myocardial infarction was assigned to 195 of the 528 patients (36.9%). Of these, 190 achieved the diagnosis within 9 hours (sensitivity 97.4%). The negative predictive value was 98.5%.Standard CK-MB mass measurements within 9 hours of arrival provided an accurate clinical assessment in > 99% of the cases. The high sensitivity and negative predictive values suggest that early diagnosis of myocardial infarction is feasible and reliable.

    View details for DOI 10.1016/j.amjms.2019.12.012

    View details for PubMedID 32039768

  • Decreased lymphatic HIF-2α accentuates lymphatic remodeling in lymphedema. The Journal of clinical investigation Jiang, X. n., Tian, W. n., Granucci, E. J., Tu, A. B., Kim, D. n., Dahms, P. n., Pasupneti, S. n., Peng, G. n., Kim, Y. n., Lim, A. H., Espinoza, F. H., Cribb, M. n., Dixon, J. B., Rockson, S. G., Semenza, G. L., Nicolls, M. R. 2020

    Abstract

    Pathologic lymphatic remodeling in lymphedema evolves during periods of tissue inflammation and hypoxia through poorly defined processes. In human and mouse lymphedema, there is a significant increase of hypoxia inducible factor (HIF)-1α, but a reduction of HIF-2α protein expression in lymphatic endothelial cells (LECs). We questioned whether dysregulated expression of these transcription factors contributes to disease pathogenesis and found that LEC-specific deletion of Hif-2α exacerbated lymphedema pathology. Even without lymphatic vascular injury, the loss of LEC-specific Hif-2α caused anatomic pathology and a functional decline in fetal and adult mice. These findings suggest that HIF-2α is an important mediator of lymphatic health. HIF-2α promoted protective phosphorylated TIE2 (p-TIE2) signaling in LECs, a process also replicated by upregulating TIE2 signaling through adenovirus-mediated angiopoietin-1 (Angpt1) gene therapy. Our study suggests that HIF-2α normally promotes healthy lymphatic homeostasis and raises the exciting possibility that restoring HIF-2α pathways in lymphedema could mitigate long-term pathology and disability.

    View details for DOI 10.1172/JCI136164

    View details for PubMedID 32673288

  • The Role of Body Mass Index in Breast Cancer-Associated Lymphedema. Lymphatic research and biology Rockson, S. G. 2020; 18 (6): 501

    View details for DOI 10.1089/lrb.2020.29095.sr

    View details for PubMedID 33351735

  • Cutaneous Pathological Changes as Quantifiable Endpoints in Human Lymphedema. Lymphatic research and biology Rockson, S. G. 2020; 18 (3): 211

    View details for DOI 10.1089/lrb.2020.29088.sr

    View details for PubMedID 32559146

  • Clinical Presentation and Imaging Attributes of the Primary Lymphedemas. Lymphatic research and biology Rockson, S. G. 2019; 17 (6): 609

    View details for DOI 10.1089/lrb.2019.29075.sr

    View details for PubMedID 31851599

  • Global guidelines trends and controversies in lower limb venous and lymphatic disease: Narrative literature revision and experts' opinions following the vWINter international meeting in Phlebology, Lymphology & Aesthetics, 23-25 January 2019. Phlebology Gianesini, S., Obi, A., Onida, S., Baccellieri, D., Bissacco, D., Borsuk, D., Campisi, C., Campisi, C. C., Cavezzi, A., Chi, Y., Chunga, J., Corda, D., Crippa, A., Davies, A., De Maeseneer, M., Diaz, J., Ferreira, J., Gasparis, A., Intriago, E., Jawien, A., Jindal, R., Kabnick, L., Latorre, A., Lee, B., Liew, N. C., Lurie, F., Meissner, M., Menegatti, E., Molteni, M., Morrison, N., Mosti, G., Narayanan, S., Pannier, F., Parsi, K., Partsch, H., Rabe, E., Raffetto, J., Raymond-Martimbeau, P., Rockson, S., Rosukhovski, D., Santiago, F. R., Schul, A., Schul, M., Shaydakov, E., Sibilla, M. G., Tessari, L., Tomaselli, F., Urbanek, T., van Rijn, M. J., Wakefield, T., Wittens, C., Zamboni, P., Bottini, O. 2019; 34 (1_suppl): 4–66

    View details for DOI 10.1177/0268355519870690

    View details for PubMedID 31495256

  • LIMPRINT: Elucidating the Global Problem of Lymphedema. Lymphatic research and biology Rockson, S. G. 2019; 17 (2): 119–20

    View details for PubMedID 30995188

  • LIMPRINT: Elucidating the Global Problem of Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2019; 17 (2): 119–20
  • Correction of complete thoracic duct obstruction with lymphovenous bypass: A case report MICROSURGERY Miller, T. J., Gilstrap, J. N., Maeda, K., Rockson, S., Nguyen, D. H. 2019; 39 (3): 255–58

    View details for DOI 10.1002/micr.30339

    View details for Web of Science ID 000462628500009

  • Lymphedema after Breast Cancer Treatment. The New England journal of medicine Rockson, S. G. 2019; 380 (7): 694

    View details for DOI 10.1056/NEJMc1817537

    View details for PubMedID 30763181

  • Lymphedema after Breast Cancer Treatment REPLY NEW ENGLAND JOURNAL OF MEDICINE Rockson, S. G. 2019; 380 (7): 694
  • Health and economic benefits of advanced pneumatic compression devices in patients with phlebolymphedema Lerman, M., Gaebler, J. A., Hoy, S., Izhakoff, J., Gullett, L., Niecko, T., Karaca-Mandic, P., O'Donnell, T., Rockson, S. G. MOSBY-ELSEVIER. 2019: 571–80

    Abstract

    Phlebolymphedema (chronic venous insufficiency-related lymphedema) is a common and costly condition. Nevertheless, there is a dearth of evidence comparing phlebolymphedema therapeutic interventions. This study sought to examine the medical resource utilization and phlebolymphedema-related cost associated with Flexitouch (FLX; Tactile Medical, Minneapolis, Minn) advanced pneumatic compression devices (APCDs) relative to conservative therapy (CONS) alone, simple pneumatic compression devices (SPCDs), and other APCDs in a representative U.S. population of phlebolymphedema patients.This was a longitudinal matched case-control analysis of deidentified private insurance claims. The study used administrative claims data from Blue Health Intelligence for the complete years 2012 through 2016. Patients were continuously enrolled for at least 18 months, diagnosed with phlebolymphedema, and received at least one claim for CONS either alone or in addition to pneumatic compression (SPCDs or APCDs). The main outcomes included direct phlebolymphedema- and sequelae-related medical resource utilization and costs.After case matching, the study included 86 patients on CONS (87 on FLX), 34 on SPCDs (23 on FLX), and 69 on other APCDs (67 on FLX). Compared with CONS, FLX was associated with 69% lower per patient per year total phlebolymphedema- and sequelae-related costs net of any pneumatic compression device-related costs ($3839 vs $12,253; P = .001). This was driven by 59% fewer mean annual hospitalizations (0.13 vs 0.32; P < .001) corresponding to 82% lower inpatient costs and 55% lower outpatient hospital costs. FLX was also associated with 52% lower outpatient physical therapy and occupational therapy costs and 56% lower other outpatient-related costs. Compared with SPCDs, FLX was associated with 85% lower total costs ($1153 vs $7449; P = .008) driven by 93% lower inpatient costs ($297 vs $4215; P = .002), 84% lower outpatient hospital costs ($368 vs $2347; P = .020), and 85% lower other outpatient-related costs ($353 vs $2313; P = .023). Compared with APCDs, FLX was associated with 53% lower total costs ($3973 vs $8436; P = .032) because of lower outpatient costs and lower rates of cellulitis (22.4% vs 44.9% of patients; P = .02).This analysis indicates significant benefits attributable to FLX compared with alternative compression therapies that can help reduce the notable economic burden of phlebolymphedema.

    View details for PubMedID 29914829

  • Modulation of Fibroblast Growth Factor Expression in Lymphedema. Lymphatic research and biology Rockson, S. G. 2019; 17 (1): 1

    View details for PubMedID 30763178

  • Modulation of Fibroblast Growth Factor Expression in Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2019; 17 (1): 1
  • The Lymphatic System in Obesity, Insulin Resistance, and Cardiovascular Diseases. Frontiers in physiology Jiang, X. n., Tian, W. n., Nicolls, M. R., Rockson, S. G. 2019; 10: 1402

    Abstract

    Obesity, insulin resistance, dyslipidemia, and hypertension are fundamental clinical manifestations of the metabolic syndrome. Studies over the last few decades have implicated chronic inflammation and microvascular remodeling in the development of obesity and insulin resistance. Newer observations, however, suggest that dysregulation of the lymphatic system underlies the development of the metabolic syndrome. This review summarizes recent advances in the field, discussing how lymphatic abnormality promotes obesity and insulin resistance, and, conversely, how the metabolic syndrome impairs lymphatic function. We also discuss lymphatic biology in metabolically dysregulated diseases, including type 2 diabetes, atherosclerosis, and myocardial infarction.

    View details for DOI 10.3389/fphys.2019.01402

    View details for PubMedID 31798464

    View details for PubMedCentralID PMC6868002

  • Author Correction: Novel mutations in PIEZO1 cause an autosomal recessive generalized lymphatic dysplasia with non-immune hydrops fetalis. Nature communications Fotiou, E. n., Martin-Almedina, S. n., Simpson, M. A., Lin, S. n., Gordon, K. n., Brice, G. n., Atton, G. n., Jeffery, I. n., Rees, D. C., Mignot, C. n., Vogt, J. n., Homfray, T. n., Snyder, M. P., Rockson, S. G., Jeffery, S. n., Mortimer, P. S., Mansour, S. n., Ostergaard, P. n. 2019; 10 (1): 1951

    Abstract

    This Article contains an error in the last sentence of the 'Variant analysis suggests they are pathogenic' section of the Results, which incorrectly reads 'No truncated PIEZO1 protein products were identified in western blot analysis in GLD1:II.3 and GLD2:II.2 (Fig. 2, Supplementary Fig. 6), suggesting that the truncated protein is not stable and therefore degraded.' This should read 'No full-size PIEZO1 protein products were identified in western blot analysis in GLD1:II.3 and GLD2:II.2 (Fig. 2, Supplementary Fig. 6); the three nonsense mutations are predicted to lead to premature termination of the protein, hence it is possible that those truncated proteins will be non-functional or even unstable and degraded.' The error has not been fixed in the PDF or HTML versions of the Article.

    View details for PubMedID 31028252

  • The Genetic Predisposition to Breast Cancer-Associated Lymphedema. Lymphatic research and biology Rockson, S. G. 2019; 17 (3): 287

    View details for DOI 10.1089/lrb.2019.29066.sr

    View details for PubMedID 31194621

  • Animal Models for the Translational Investigation of Lymphedema. Lymphatic research and biology Rockson, S. G. 2019

    View details for DOI 10.1089/lrb.2019.29069.sr

    View details for PubMedID 31361584

  • Progress in the Approach to Lymphatic Vascular Malformation. Lymphatic research and biology Rockson, S. G. 2019; 17 (5): 495

    View details for DOI 10.1089/lrb.2019.29071.sr

    View details for PubMedID 31618140

  • Biomarker Assessment in Lymphedema of the Head and Neck LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2018; 16 (6): 497
  • Diagnosis of Early and Subclinical Lymphedema Following Breast Cancer. Lymphatic research and biology Rockson, S. G. 2018; 16 (5): 425

    View details for PubMedID 30332352

  • Diagnosis of Early and Subclinical Lymphedema Following Breast Cancer LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2018; 16 (5): 425
  • Yellow Nail Syndrome: A Mystery, Partially Solved. Lymphatic research and biology Rockson, S. G. 2018; 16 (4): 329

    View details for PubMedID 30130157

  • Yellow Nail Syndrome: A Mystery, Partially Solved LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2018; 16 (4): 329
  • Correction of complete thoracic duct obstruction with lymphovenous bypass: A case report. Microsurgery Miller, T. J., Gilstrap, J. N., Maeda, K., Rockson, S., Nguyen, D. H. 2018

    Abstract

    Thoracic duct injury can be a devastating injury with disruption of lymphatic flow leading to potentially chylothorax and/or severe lymphedema. Standard treatment modalities include thoracic duct ligation or embolization for chylothorax, but treatment options to date are few for resultant lymphedema. In this case report, we describe lymphaticovenous bypass of the thoracic duct to the jugular venous system in a 21-year-old male with secondary lymphedema after iatrogenic thoracic duct injury. The patient experienced improvement of lymphedema symptoms including decreased weight and limb girth as well as normalization of serum markers indicating improved lymphatic delivery to the venous system. Lymphangiogram at 3 months post op demonstrated patency of the lymphaticovenous anastomoses. At 6-month follow-up, the patient had returned to his preoperative level of activity and showed continued improvement of his lymphedema symptoms. Lymphovenous bypass of the thoracic duct may be an effective technique to treat secondary lymphedema from thoracic duct obstruction, though further studies are required to determine long-term efficacy.

    View details for PubMedID 29974499

  • Prospective Experimental Study of Microvascular Reconstruction in Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2018; 16 (3): 233

    View details for PubMedID 29912665

  • Biotechnologies toward Mitigating, Curing, and Ultimately Preventing Edema through Compression Therapy TRENDS IN BIOTECHNOLOGY Hageman, D. J., Wu, S., Kilbreath, S., Rockson, S. G., Wang, C., Tate, M. 2018; 36 (5): 537–48

    Abstract

    For a century-old problem, edema and its treatment have gone remarkably unnoticed by the biomedical community. Given the prevalence of lymphedema and its debilitating repercussions, there is an acute need for both efficacy-based measures and clinical standards to guide compression garment design and therapeutic application. This review outlines the current state of the art in compression treatment and suggests an integrated biomedical engineering approach going forward. Characterizing the pressure gradient profiles of commercial compression sleeves is necessary to better understand the role of compression treatment in the mitigation of swelling. Integration of pressure sensor technologies with advanced materials design and manufacture provides a critical path not only to elucidate the mechanisms of but also to improve on current compression-based therapies and associated therapeutic devices.

    View details for PubMedID 29606499

  • Lymphatics and the Pathogenesis of Hypertension LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2018; 16 (2): 133

    View details for PubMedID 29659335

  • Regulatory T Cells Mediate Local Immunosuppression in Lymphedema JOURNAL OF INVESTIGATIVE DERMATOLOGY Nores, G., Ly, C. L., Savetsky, I. L., Kataru, R. P., Ghanta, S., Hespe, G. E., Rockson, S. G., Mehrara, B. J. 2018; 138 (2): 325–35

    Abstract

    Patients who suffer from lymphedema have impaired immunity and, as a result, are at an increased risk for infections. Furthermore, previous studies have shown that lymphadenectomy impairs acquisition of adaptive immune responses and antibody production in response to foreign antigens. Although it is clear that antigen presentation in lymph nodes plays a key role in adaptive immunity, the cellular mechanisms that regulate impaired immune responses in patients with lymphedema or following lymphatic injury remain unknown. We have previously found that axillary lymph node dissection, both clinically and in a mouse model, results in a marked increase in the number of regulatory T cells in the ipsilateral limb. In this study, we focus on the role of regulatory T cells in immunosuppression and show that regulatory T-cell proliferation in tissues distal to site of lymphatic injury contributes to impaired innate and adaptive immune responses. More importantly, using Foxp3-DTR transgenic mice, we show that depletion of regulatory T cells in the setting of lymphatic injury restores these critical immune-mediated responses. These findings provide additional evidence that immune responses following lymphatic injury play a key role in mediating the pathology of lymphedema.

    View details for PubMedID 28942366

    View details for PubMedCentralID PMC5794510

  • Growing Insights into Breast Cancer-Related Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2018; 16 (1): 1

    View details for PubMedID 29432070

  • Lymphatic Medicine: Paradoxically and Unnecessarily Ignored LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2017; 15 (4): 315–16

    View details for PubMedID 29252138

    View details for PubMedCentralID PMC5787933

  • Considerations for Clinicians in the Diagnosis, Prevention, and Treatment of Breast Cancer-Related Lymphedema: Recommendations from a Multidisciplinary Expert ASBrS Panel ANNALS OF SURGICAL ONCOLOGY McLaughlin, S. A., Staley, A. C., Vicini, F., Thiruchelvam, P., Hutchison, N. A., Mendez, J., MacNeill, F., Rockson, S. G., DeSnyder, S. M., Klimberg, S., Alatriste, M., Boccardo, F., Smith, M. L., Feldman, S. M. 2017; 24 (10): 2818–26

    View details for PubMedID 28766232

  • Considerations for Clinicians in the Diagnosis, Prevention, and Treatment of Breast Cancer-Related Lymphedema, Recommendations from an Expert Panel: Part 2: Preventive and Therapeutic Options ANNALS OF SURGICAL ONCOLOGY McLaughlin, S. A., DeSnyder, S. M., Klimberg, S., Alatriste, M., Boccardo, F., Smith, M. L., Staley, A. C., Thiruchelvam, P. R., Hutchison, N. A., Mendez, J., MacNeill, F., Vicini, F., Rockson, S. G., Feldman, S. M. 2017; 24 (10): 2827–35

    View details for PubMedID 28766218

  • A Role for Near Infrared Fluorescent Imaging in the Evaluation of Lymphatic Function LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2017; 15 (3): 203

    View details for PubMedID 28937922

  • A Comparison of Programmable and Non-Programmable Compression Devices for Treatment of Lymphedema Using an Administrative Health Outcomes Dataset. British journal of dermatology Karaca-Mandic, P., Hirsch, A. T., Rockson, S. G., Ridner, S. H. 2017

    Abstract

    Patients with lymphedema suffer lifelong swelling and recurrent cellulitis despite use of complete decongestive therapy. Pneumatic compression devices (PCDs), including non-programmable and programmable devices that meet individual patient needs, support long term self-care in the home. Yet, to date, no direct comparison of their relative benefits has been available.Patients who acquired either a non-programmable device (NP-PCD) or a dynamic pressure programmable device (P-PCD; Flexitouch(®) ) were evaluated to compare associated clinical and health utilization outcomes pre/post-device acquisition.Retrospective analysis of de-identified administrative claims from 2007 through 2013 of a large United States insurer. The study populations were defined pre hoc as distinct cancer- and non-cancer-related lymphedema cohorts. Outcome variables included rates of lymphedema-related cellulitis, manual therapy use, outpatient services, and inpatient hospitalizations. Multivariate regression analysis was performed to: (1) compare outcomes for the 12 months pre- and post-device acquisition and (2) compare these two device types for their treatment-associated benefits.The sample consisted of 1,013 NP-PCD and 718 P-PCD recipients. Compared with the NP-PCD group, P-PCD patients' baseline cellulitis rate was higher, while their post-device cellulitis rate was lower. In the cancer cohort, the NP-PCD group had a 53% reduction in episodes of cellulitis (from 17.9% to 8.5%), compared to a greater 79% reduction in the P-PCD group (from 23.7% to 5.0%) (p<0.001). In the non-cancer cohort, the P-PCD group also experienced a larger 76% decline (from 31.7% to 7.4%) vs. 54% decline (from 22.9% to 10.6%) in cellulitis rates (p=0.003). Outpatient service use reduced in both device groups, with greater reductions observed in P-PCD group. Both device groups experienced reductions in manual therapy use. Inpatient hospitalizations were largely stable with reductions observed only in the non-cancer cohort of the P-PCD group.P-PCD receipt was associated with superior lymphedema-related health outcomes and reductions in cellulitis. This article is protected by copyright. All rights reserved.

    View details for DOI 10.1111/bjd.15699

    View details for PubMedID 28573790

  • Lymphatic Endothelial Cells: Mechanical Stress, Cytokines, Fibrosis, and Age LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2017; 15 (2): 129

    View details for PubMedID 28617647

  • Isolated Human Lymphatic Vessels and Lymphatic Endothelial Cells LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2017; 15 (1): 1

    View details for PubMedID 28323569

  • Lymphedema in Head and Neck Cancer LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2016; 14 (4): 197

    View details for PubMedID 27997312

  • Pregnancy Complicated by Gorham-Stout Disease and Refractory Chylothorax. AJP reports Hellyer, J., Oliver-Allen, H., Shafiq, M., Tolani, A., Druzin, M., Jeng, M., Rockson, S., Lowsky, R. 2016; 6 (4): e355-e358

    Abstract

    Introduction Gorham-Stout Disease (GSD) is a rare disorder of bony destruction due to lymphangiomatosis, and is often triggered by hormones. One complication of GSD is the development of chylothorax, which carries a high mortality rate. Very little experience has been published to guide management in GSD during pregnancy to optimize both fetal and maternal health. Case Study A 20-year-old woman with known GSD presented with shortness of breath at 18 weeks of pregnancy, due to bilateral chylothoraces which required daily drainage. To minimize chylous fluid formation, she was placed on bowel rest with total parenteral nutrition (limiting lipid intake) and received octreotide to decrease splanchnic blood flow and chylous fluid drainage. Treatment options were limited due to her pregnancy. Twice daily home chest tube drainage of a single lung cavity, total parenteral nutrition, octreotide, and albumin infusions allowed successful delivery of a healthy 37 weeks' gestation infant by cesarean delivery. Discussion This case illustrates the management of a rare clinical disease of bone resorption and lymphangiomatosis complicated by bilateral, refractory chylothoraces, triggered by pregnancy, in whom treatment options are limited, and the need for a multidisciplinary health care team to ensure successful maternal and fetal outcomes.

    View details for PubMedID 27708981

  • Erratum: Pregnancy Complicated by Gorham-Stout Disease and Refractory Chylothorax. AJP reports Hellyer, J., Oliver-Allen, H., Shafiq, M., Tolani, A., Druzin, M., Jeng, M., Rockson, S., Lowsky, R. 2016; 6 (4)

    Abstract

    [This corrects the article DOI: 10.1055/s-0036-1593443.].

    View details for PubMedID 27822433

  • Lymphedema Is a Disease of the Skin LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2016; 14 (3): 123

    View details for PubMedID 27631580

  • EPHB4 kinase-inactivating mutations cause autosomal dominant lymphatic-related hydrops fetalis. journal of clinical investigation Martin-Almedina, S., Martinez-Corral, I., Holdhus, R., Vicente, A., Fotiou, E., Lin, S., Petersen, K., Simpson, M. A., Hoischen, A., Gilissen, C., Jeffery, H., Atton, G., Karapouliou, C., Brice, G., Gordon, K., Wiseman, J. W., Wedin, M., Rockson, S. G., Jeffery, S., Mortimer, P. S., Snyder, M. P., Berland, S., Mansour, S., Makinen, T., Ostergaard, P. 2016; 126 (8): 3080-3088

    Abstract

    Hydrops fetalis describes fluid accumulation in at least 2 fetal compartments, including abdominal cavities, pleura, and pericardium, or in body tissue. The majority of hydrops fetalis cases are nonimmune conditions that present with generalized edema of the fetus, and approximately 15% of these nonimmune cases result from a lymphatic abnormality. Here, we have identified an autosomal dominant, inherited form of lymphatic-related (nonimmune) hydrops fetalis (LRHF). Independent exome sequencing projects on 2 families with a history of in utero and neonatal deaths associated with nonimmune hydrops fetalis uncovered 2 heterozygous missense variants in the gene encoding Eph receptor B4 (EPHB4). Biochemical analysis determined that the mutant EPHB4 proteins are devoid of tyrosine kinase activity, indicating that loss of EPHB4 signaling contributes to LRHF pathogenesis. Further, inactivation of Ephb4 in lymphatic endothelial cells of developing mouse embryos led to defective lymphovenous valve formation and consequent subcutaneous edema. Together, these findings identify EPHB4 as a critical regulator of early lymphatic vascular development and demonstrate that mutations in the gene can cause an autosomal dominant form of LRHF that is associated with a high mortality rate.

    View details for DOI 10.1172/JCI85794

    View details for PubMedID 27400125

    View details for PubMedCentralID PMC4966301

  • Physiological Mechanisms that Predispose to the Development of Breast Cancer-Associated Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2016; 14 (2): 49

    View details for PubMedID 27309031

  • Ultrasonography in the Evaluation of Breast Cancer-Related Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2016; 14 (1): 1

    View details for PubMedID 26982710

  • Lymphedema VASCULAR MEDICINE Rockson, S. G. 2016; 21 (1): 77–81

    View details for DOI 10.1177/1358863X15620852

    View details for Web of Science ID 000369075500013

    View details for PubMedID 26819350

  • Modeling the Lymphatics LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2015; 13 (4): 233

    View details for PubMedID 26683025

  • Detecting Lymphedema: Bioimpedance Spectroscopy and the Tissue Dielectric Constant LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2015; 13 (3): 169

    View details for PubMedID 26359689

  • IUA-ISVI consensus for diagnosis guideline of chronic lymphedema of the limbs. International angiology Lee, B. B., Antignani, P. L., Baroncelli, T. A., Boccardo, F. M., Brorson, H., Campisi, C., Damstra, R. J., Flour, M., Giannoukas, A., Laredo, J., Liu, N. F., Michelini, S., Piller, N., Rockson, S. G., Scuderi, A., Szolnoky, G., Yamamoto, T. 2015; 34 (4): 311-332

    View details for PubMedID 24699525

  • Dietary Sodium and Lymphatic Contractile Activity LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2015; 13 (2): 75

    View details for PubMedID 26091402

  • Detection of Tissue Edema in Breast Cancer-Associated Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2015; 13 (1): 1

    View details for PubMedID 25768054

  • Novel mutations in PIEZO1 cause an autosomal recessive generalized lymphatic dysplasia with non-immune hydrops fetalis. Nature communications Fotiou, E., Martin-Almedina, S., Simpson, M. A., Lin, S., Gordon, K., Brice, G., Atton, G., Jeffery, I., Rees, D. C., Mignot, C., Vogt, J., Homfray, T., Snyder, M. P., Rockson, S. G., Jeffery, S., Mortimer, P. S., Mansour, S., Ostergaard, P. 2015; 6: 8085-?

    View details for DOI 10.1038/ncomms9085

    View details for PubMedID 26333996

  • Lymphangiogenesis, the CCR7 Receptor, and Human Atherosclerosis LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2014; 12 (4): 215

    View details for PubMedID 25495380

  • Inflammatory Cytokines and the Lymphatic Endothelium LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2014; 12 (3): 123

    View details for PubMedID 25229431

  • The Role of Lymph Node Irradiation in the Pathogenesis of Acquired Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2014; 12 (2): 65

    View details for PubMedID 24927064

  • IL-6 regulates adipose deposition and homeostasis in lymphedema AMERICAN JOURNAL OF PHYSIOLOGY-HEART AND CIRCULATORY PHYSIOLOGY Cuzzone, D. A., Weitman, E. S., Albano, N. J., Ghanta, S., Savetsky, I. L., Gardenier, J. C., Joseph, W. J., Torrisi, J. S., Bromberg, J. F., Olszewski, W. L., Rockson, S. G., Mehrara, B. J. 2014; 306 (10)

    Abstract

    Lymphedema (LE) is a morbid disease characterized by chronic limb swelling and adipose deposition. Although it is clear that lymphatic injury is necessary for this pathology, the mechanisms that underlie lymphedema remain unknown. IL-6 is a known regulator of adipose homeostasis in obesity and has been shown to be increased in primary and secondary models of lymphedema. Therefore, the purpose of this study was to determine the role of IL-6 in adipose deposition in lymphedema. The expression of IL-6 was analyzed in clinical tissue specimens and serum from patients with or without LE, as well as in two mouse models of lymphatic injury. In addition, we analyzed IL-6 expression/adipose deposition in mice deficient in CD4(+) cells (CD4KO) or IL-6 expression (IL-6KO) or mice treated with a small molecule inhibitor of IL-6 or CD4 depleting antibodies to determine how IL-6 expression is regulated and the effect of changes in IL-6 expression on adipose deposition after lymphatic injury. Patients with LE and mice treated with lymphatic excision of the tail had significantly elevated tissue and serum expression of IL-6 and its downstream mediator. The expression of IL-6 was associated with adipose deposition and CD4(+) inflammation and was markedly decreased in CD4KO mice. Loss of IL-6 function resulted in significantly increased adipose deposition after tail lymphatic injury. Our findings suggest that IL-6 is increased as a result of adipose deposition and CD4(+) cell inflammation in lymphedema. In addition, our study suggests that IL-6 expression in lymphedema acts to limit adipose accumulation.

    View details for DOI 10.1152/ajpheart.01019.2013

    View details for PubMedID 24633552

  • Acquired Lymphedema: Abnormal Fluid Clearance Engenders Tissue Remodeling LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2014; 12 (1): 1

    View details for PubMedID 24650108

  • Essential Role of Apelin Signaling During Lymphatic Development in Zebrafish ARTERIOSCLEROSIS THROMBOSIS AND VASCULAR BIOLOGY Kim, J., Kang, Y., Kim, J., Papangeli, I., Kang, H., Wu, J., Park, H., Nadelmann, E., Rockson, S. G., Chun, H. J., Jin, S. 2014; 34 (2): 338-345

    Abstract

    Apelin and its cognate receptor Aplnr/Apj are essential for diverse biological processes. However, the function of Apelin signaling in lymphatic development remains to be identified, despite the preferential expression of Apelin and Aplnr within developing blood and lymphatic endothelial cells in vertebrates. In this report, we aim to delineate the functions of Apelin signaling during lymphatic development.We investigated the functions of Apelin signaling during lymphatic development using zebrafish embryos and found that attenuation of Apelin signaling substantially decreased the formation of the parachordal vessel and the number of lymphatic endothelial cells within the developing thoracic duct, indicating an essential role of Apelin signaling during the early phase of lymphatic development. Mechanistically, we found that abrogation of Apelin signaling selectively attenuates lymphatic endothelial serine-threonine kinase Akt 1/2 phosphorylation without affecting the phosphorylation status of extracellular signal-regulated kinase 1/2. Moreover, lymphatic abnormalities caused by the reduction of Apelin signaling were significantly exacerbated by the concomitant partial inhibition of serine-threonine kinase Akt/protein kinase B signaling. Apelin and vascular endothelial growth factor-C (VEGF-C) signaling provide a nonredundant activation of serine-threonine kinase Akt/protein kinase B during lymphatic development because overexpression of VEGF-C or apelin was unable to rescue the lymphatic defects caused by the lack of Apelin or VEGF-C, respectively.Taken together, our data present compelling evidence suggesting that Apelin signaling regulates lymphatic development by promoting serine-threonine kinase Akt/protein kinase B activity in a VEGF-C/VEGF receptor 3-independent manner during zebrafish embryogenesis.

    View details for DOI 10.1161/ATVBAHA.113.302785

    View details for PubMedID 24311379

  • Diagnosis and Treatment of Primary Lymphedema Consensus Document of the International Union of Phlebology (IUP)-2013 INTERNATIONAL ANGIOLOGY Lee, B. B., Andrade, M., Antignani, P. L., Boccardo, F., Bunke, N., Campisi, C., Damstra, R., Flour, M., Forner-Cordero, I., Gloviczki, P., Laredo, J., Partsch, H., Piller, N., Michelini, S., Mortimer, P., Rabe, E., Rockson, S., Scuderi, A., Szolnoky, G., Villavicencio, J. L. 2013; 32 (6): 541-574

    Abstract

    Primary lymphedema can be managed effectively as a form of chronic lymphedema by a sequenced and targeted treatment and management program based around a combination of Decongestive Lymphatic Therapy (DLT) with compression therapy, when the latter is desired as an adjunct to DLT. Treatment in the maintenance phase should include compression garments, self-management, including self-massage, meticulous personal hygiene and skin care, in addition to lymphtransport-promoting excercises and activities, and, if desired, pneumatic compression therapy applied in the home. When conservative treatment fails, or gives sub-optimal outcomes, the management of primary lymphedema can be improved, where appropriate, with the proper addition of surgical interventions, either reconstructive or ablative. These two surgical therapies can be more effective when fully integrated with manual lymphatic drainage (MLD)-based DLT postoperatively. Compliance with a long-term commitment to MLD/DLT and particularly compression postoperatively is a critical factor in determining the success of any new treatment strategy involving either reconstructive or palliative surgery. The future of management of primary lymphedema has never been brighter with the new prospect of gene-and perhaps stem-cell oriented management.

    View details for Web of Science ID 000331344500001

    View details for PubMedID 24212289

  • Tissue Changes, Bioimpedance, and Acquired Lymphedema LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2013; 11 (4): 195

    View details for PubMedID 24364841

  • Lymphatics: Where the Circulation Meets the Immune System LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2013; 11 (3): 115-115

    View details for DOI 10.1089/lrb.2013.1131

    View details for PubMedID 24024578

  • Assessing extracellular fluid volume in breast cancer lymphedema. Lymphatic research and biology Rockson, S. G. 2013; 11 (2): 65-?

    View details for DOI 10.1089/lrb.2013.1122

    View details for PubMedID 23772714

  • Th2 differentiation is necessary for soft tissue fibrosis and lymphatic dysfunction resulting from lymphedema FASEB JOURNAL Avraham, T., Zampell, J. C., Yan, A., Elhadad, S., Weitman, E. S., Rockson, S. G., Bromberg, J., Mehrara, B. J. 2013; 27 (3): 1114-1126

    Abstract

    Lymphedema is a dreaded complication of cancer treatment. However, despite the fact that >5 million Americans are affected by this disorder, the development of effective treatments is limited by the fact that the pathology of lymphedema remains unknown. The purpose of these studies was to determine the role of inflammatory responses in lymphedema pathology. Using mouse models of lymphedema, as well as clinical lymphedema specimens, we show that lymphatic stasis results in a CD4 T-cell inflammation and T-helper 2 (Th2) differentiation. Using mice deficient in T cells or CD4 cells, we show that this inflammatory response is necessary for the pathological changes of lymphedema, including fibrosis, adipose deposition, and lymphatic dysfunction. Further, we show that inhibition of Th2 differentiation using interleukin-4 (IL-4) or IL-13 blockade prevents initiation and progression of lymphedema by decreasing tissue fibrosis and significantly improving lymphatic function, independent of lymphangiogenic growth factors. We show that CD4 inflammation is a critical regulator of tissue fibrosis and lymphatic dysfunction in lymphedema and that inhibition of Th2 differentiation markedly improves lymphatic function independent of lymphangiogenic cytokine expression. Notably, preventing and/or reversing the development of pathological tissue changes that occur in lymphedema may be a viable treatment strategy for this disorder.

    View details for DOI 10.1096/fj.12-222695

    View details for Web of Science ID 000315585200025

    View details for PubMedID 23193171

    View details for PubMedCentralID PMC3574290

  • The Aging Lymphatics Become More Mature LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2013; 11 (1): 1-1

    View details for DOI 10.1089/lrb.2013.1111

    View details for Web of Science ID 000316735400001

    View details for PubMedID 23531178

  • Experimental lymphedema: can cellular therapies augment the therapeutic potential for lymphangiogenesis? Journal of the American Heart Association Rockson, S. G. 2012; 1 (4)

    View details for DOI 10.1161/JAHA.112.003400

    View details for PubMedID 23130177

  • Lack of Significant Interactions Between Clopidogrel and Proton Pump Inhibitor Therapy: Meta-Analysis of Existing Literature DIGESTIVE DISEASES AND SCIENCES Gerson, L. B., McMahon, D., Olkin, I., Stave, C., Rockson, S. G. 2012; 57 (5): 1304-1313

    Abstract

    Published data regarding the effect of concomitant clopidogrel and proton pump inhibitor (PPI) therapy on cardiovascular outcomes have been conflicting.To perform an updated meta-analysis in order to determine changes in risk differences (RD) between primary and secondary outcome analyses.Primary analysis was based on definite vascular outcomes, including all cause mortality, cardiac death, myocardial infarction, and/or stroke. Secondary analysis also incorporated probable cardiac events, which included re-hospitalization for cardiac symptoms or revascularization procedures. RD were combined using a random-effects model.We reviewed 1,204 publications of which 26 studies (16 published articles, 10 abstracts) met inclusion criteria. The meta-analysis of outcomes from the two randomized controlled trials did not show an increased risk (RD 0.0, 95% CI -0.01, 0.01) for adverse outcomes. The meta-analysis of primary outcomes showed a RD of 0.02 (95% CI 0.01, 0.03) for all studies. The meta-analysis for secondary outcomes yielded a RD of 0.02 (95% CI 0.01-0.04) based on 19 published papers and abstracts. When primary and secondary outcomes were combined, the meta-analysis for published papers yielded an overall RD of 0.05 (95% CI 0.03-0.06).In patients using concomitant clopidogrel and PPI therapy, the risk of adverse cardiac outcomes was 0% based on data from well-controlled randomized trials. Data from retrospective studies and the addition of probable vascular events significantly increased the RD estimates, likely due to lack of adjustment for potential confounders.

    View details for DOI 10.1007/s10620-011-2007-1

    View details for PubMedID 22198703

  • Update on the biology and treatment of lymphedema. Current treatment options in cardiovascular medicine Rockson, S. G. 2012; 14 (2): 184-192

    Abstract

    OPINION STATEMENT: The past decade has produced an explosion of insights into lymphatic vascular development and structural biology and, in parallel, into the function of the lymphatics in health and in disease. In lymphedema, there is a spectrum that extends from primary (heritable) to acquired causes of disease. The diagnosis of lymphatic edema implicates a very specific treatment approach that is predicated upon the favorable impact of physiotherapy upon lymph flow and protein clearance from the edematous zones of the body. The recognition of the unique biology that accompanies lymphatic causes of edema has stimulated new research directions that are likely to translate into exciting new pharmacologic and molecular approaches to diagnosis and treatment.

    View details for DOI 10.1007/s11936-012-0170-0

    View details for PubMedID 22382848

  • Cancer Is Part of the Lymphatic Continuum LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2012; 10 (3): 95-95

    View details for DOI 10.1089/lrb.2012.1031

    View details for Web of Science ID 000309054500001

    View details for PubMedID 22984903

  • The Lymphatic Biology of Aging LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2012; 10 (2): 45-45

    View details for DOI 10.1089/lrb.2012.1021

    View details for Web of Science ID 000305865400001

    View details for PubMedID 22720660

  • Reflections on a Decade of Lymphatic Research and Biology LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2012; 10 (1): 1-1

    View details for DOI 10.1089/lrb.2012.1011

    View details for Web of Science ID 000302275800001

    View details for PubMedID 22439852

  • Angiogenesis, Lymphangiogenesis, and Inflammation LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2012; 10 (4): 151-151

    View details for DOI 10.1089/lrb.2012.1041

    View details for Web of Science ID 000312461100001

    View details for PubMedID 23240955

  • Temporal and spatial patterns of endogenous danger signal expression after wound healing and in response to lymphedema AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY Zampell, J. C., Yan, A., Avraham, T., Andrade, V., Malliaris, S., Aschen, S., Rockson, S. G., Mehrara, B. J. 2011; 300 (5): C1107-C1121

    Abstract

    While acute tissue injury potently induces endogenous danger signal expression, the role of these molecules in chronic wound healing and lymphedema is undefined. The purpose of this study was to determine the spatial and temporal expression patterns of the endogenous danger signals high-mobility group box 1 (HMGB1) and heat shock protein (HSP)70 during wound healing and chronic lymphatic fluid stasis. In a surgical mouse tail model of tissue injury and lymphedema, HMGB1 and HSP70 expression occurred along a spatial gradient relative to the site of injury, with peak expression at the wound and greater than twofold reduced expression within 5 mm (P < 0.05). Expression primarily occurred in cells native to injured tissue. In particular, HMGB1 was highly expressed by lymphatic endothelial cells (>40% positivity; twofold increase in chronic inflammation, P < 0.001). We found similar findings using a peritoneal inflammation model. Interestingly, upregulation of HMGB1 (2.2-fold), HSP70 (1.4-fold), and nuclear factor (NF)-κβ activation persisted at least 6 wk postoperatively only in lymphedematous tissues. Similarly, we found upregulation of endogenous danger signals in soft tissue of the arm after axillary lymphadenectomy in a mouse model and in matched biopsy samples obtained from patients with secondary lymphedema comparing normal to lymphedematous arms (2.4-fold increased HMGB1, 1.9-fold increased HSP70; P < 0.01). Finally, HMGB1 blockade significantly reduced inflammatory lymphangiogenesis within inflamed draining lymph nodes (35% reduction, P < 0.01). In conclusion, HMGB1 and HSP70 are expressed along spatial gradients and upregulated in chronic lymphatic fluid stasis. Furthermore, acute expression of endogenous danger signals may play a role in inflammatory lymphangiogenesis.

    View details for DOI 10.1152/ajpcell.00378.2010

    View details for Web of Science ID 000289884300017

    View details for PubMedID 21248077

    View details for PubMedCentralID PMC3093946

  • Stress-induced cardiomyopathy associated with a transfusion reaction: A case of potential crosstalk between the histaminic and adrenergic systems EXPERIMENTAL & CLINICAL CARDIOLOGY Zhou, J. Q., Choe, E., Ang, L., Schnittger, I., Rockson, S. G., Tremmel, J. A., Haddad, F. 2011; 16 (1): 30-32

    Abstract

    The adrenergic and histaminergic systems have been reported to have analogous effects on the heart. A case of transient ventricular dysfunction with echocardiographic findings characteristic of stress-induced cardiomyopathy (also known as takotsubo cardiomyopathy) in a patient who had an urticarial transfusion reaction is described. The effect of histamine on ventricular function and its interaction with the adrenergic system are discussed.

    View details for Web of Science ID 000300518800008

    View details for PubMedID 21523205

    View details for PubMedCentralID PMC3076164

  • Animal Models for the Mechanistic Study of Systemic Lymphangiomatosis LYMPHATIC RESEARCH AND BIOLOGY Rockson, S. G. 2011; 9 (4): 195-199

    Abstract

    The systematic study of focused animal models has produced an explosion of information regarding the mechanisms governing lymphatic development and the diseases associated with lymphatic dysfunction. Nevertheless, the pathogenesis of systemic lymphangiomatosis has, thus far, eluded mechanistic comprehension. In this review, recent molecular advances in lymphatic vascular development are considered within the context of the animal models that have produced evolving insights. The emerging role of the zebrafish within lymphatic investigation is discussed. Specific models of the human disease pathology are considered in detail. While much has been learned about the molecular framework that surrounds normal lymphatic vascular development, the defect responsible for systemic lymphangiomatosis remains elusive. Development of more robust, recapitulative models will also be invaluable to investigate new and emerging therapeutics for the often devastating disease of systemic lymphangiomatosis.

    View details for DOI 10.1089/lrb.2011.0017

    View details for PubMedID 22196285

  • Managing Breast Cancer-Associated Lymphedema BREAST SURGICAL TECHNIQUES AND INTERDISCIPLINARY MANAGEMENT Rockson, S. G., Dirbas, F. M., ScottConner, C. E. 2011: 1015–27
  • Embryology of the Lymphatic System and Lymphangiogenesis LYMPHEDEMA: A CONCISE COMPENDIUM OF THEORY AND PRACTICE Rockson, S. G., Lee, B. B., Bergan, J., Rockson, S. G. 2011: 43–48
  • Blockade of Transforming Growth Factor-beta 1 Accelerates Lymphatic Regeneration during Wound Repair AMERICAN JOURNAL OF PATHOLOGY Avraham, T., Daluvoy, S., Zampell, J., Yan, A., Haviv, Y. S., Rockson, S. G., Mehrara, B. J. 2010; 177 (6): 3202-3214

    Abstract

    Lymphedema is a complication of cancer treatment occurring in approximately 50% of patients who undergo lymph node resection. Despite its prevalence, the etiology of this disorder remains unknown. In this study, we determined the effect of soft tissue fibrosis on lymphatic function and the role of transforming growth factor (TGF)-β1 in the regulation of this response. We determined TGF-β expression patterns in matched biopsy specimens collected from lymphedematous and normal limbs of patients with secondary lymphedema. To determine the role of TGF-β in regulating tissue fibrosis, we used a mouse model of lymphedema and inhibited TGF-β function either systemically with a monoclonal antibody or locally by using a soluble, defective TGF-β receptor. Lymphedematous tissue demonstrated a nearly threefold increase in the number of cells that stained for TGF-β1. TGF-β inhibition markedly decreased tissue fibrosis, increased lymphangiogenesis, and improved lymphatic function compared with controls. In addition, inhibition of TGF-β not only decreased TGF-β expression in lymphedematous tissues, but also diminished inflammation, migration of T-helper type 2 (Th2) cells, and expression of profibrotic Th2 cytokines. Similarly, systemic depletion of T-cells markedly decreased TGF-β expression in tail tissues. Inhibition of TGF-β function promoted lymphatic regeneration, decreased tissue fibrosis, decreased chronic inflammation and Th2 cell migration, and improved lymphatic function. The use of these strategies may represent a novel means of preventing lymphedema after lymph node resection.

    View details for DOI 10.2353/ajpath.2010.100594

    View details for Web of Science ID 000285369800050

    View details for PubMedID 21056998

    View details for PubMedCentralID PMC2993295

  • Current concepts and future directions in the diagnosis and management of lymphatic vascular disease VASCULAR MEDICINE Rockson, S. G. 2010; 15 (3): 223-231

    Abstract

    Despite the central, complex role for the lymphatic system in the maintenance of human health, the biology of this important and complex vasculature has been relatively under-investigated. However, the last decade has witnessed a substantial growth in the elucidation of lymphatic structural biology and the function of this system in health and in disease. These newly gained insights can be used to formulate our evolving concepts about the diagnostic and therapeutic approaches to patients with lymphatic vascular disorders. In lymphedema, there is a spectrum of disease that extends from primary (heritable) to secondary (acquired) causes. Once detected, the presence of lymphatic edema mandates very specific modalities of intervention, predominated by physiotherapeutic techniques. In addition, a physiological basis for adjunctive, intermittent pneumatic compression has been established, and these modalities may be indicated in selected patient populations. The acknowledgement of a unique biology in lymphatic edemas is, increasingly, guiding research efforts within this field. Increasing investigative attention is being directed toward animal models of lymphatic vascular disease. As insight into the complex biology of the lymphatic vasculature continues to expand through focused biomedical investigation, the translation of these mechanistic insights into targeted, rationally conceived therapeutics will become increasingly feasible.

    View details for DOI 10.1177/1358863X10364553

    View details for PubMedID 20483987

  • Causes and consequences of lymphatic disease Conference on Lymphatics in the Digestive System - Physiology, Health, and Disease Rockson, S. G. WILEY-BLACKWELL. 2010: E2–E6

    Abstract

    The visceral manifestations of lymphatic disorders (lymphangiomatosis and lymphangiectasia) are particularly severe. Any pathology of the lymphatic vasculature, whether superficial or internal, regional, or systemic, is predominated by the appearance of lymphedema, the characteristic form of tissue edema that occurs when lymphatic dysfunction supervenes. Disease manifestations may include dysregulation of body fluid homeostasis, immune traffic impairment, and disturbances of lipid and protein reabsorption from the gut lumen. The appearance of lymphatic edema invokes complex biological alterations. Many of these changes seem to relate uniquely to chronic lymphatic edema, including a profound stimulus to collagen and adipose deposition. Despite the recent advances in our understanding of these disorders, substantial knowledge gaps remain; these gaps inhibit our ability to accurately identify, categorize, treat, and prevent these diseases. Future diagnostic, therapeutic, and reproductive decisions for affected individuals require an accurate knowledge of the clinical and laboratory presentation, mode of inheritance, treatment response, outcomes, and prognosis.

    View details for PubMedID 20961302

  • Introduction LYMPHATICS IN THE DIGESTIVE SYSTEM: PHYSIOLOGY, HEALTH, AND DISEASE Rockson, S. G., Rockson, S. 2010; 1207: E1
  • Lymphatic research: past, present, and future. Lymphatic research and biology Rockson, S. G. 2009; 7 (4): 183-187

    View details for DOI 10.1089/lrb.2009.7402

    View details for PubMedID 20143916

  • Appropriate Secondary Prevention of Acute Atherothrombotic Events and Strategies to Improve Guideline Adherence POSTGRADUATE MEDICINE Rockson, S. G. 2009; 121 (1): 25-39

    Abstract

    The use of guideline-recommended secondary prevention measures is essential for reducing the risk of subsequent events and mortality in patients who have survived an acute atherothrombotic event or have peripheral arterial disease. Although initial hospitalization provides an ideal environment to initiate such therapies, implementation of effective longterm prevention strategies is hindered by the absence of a systematic approach. In general, evidence-based clinical practice guidelines recommend antiplatelet therapy as a cornerstone of post-discharge secondary prevention, in addition to preventive measures targeting risk factors such as hypertension, dyslipidemia, cigarette smoking, and physical inactivity. Observational data indicate that, although there has been improvement over time, current utilization of guideline-recommended post-discharge treatment remains suboptimal. Recognizing the importance of a systematic approach to discharge planning, numerous hospital-based initiatives have been established. In conjunction with effective lines of communication between hospital and primary care teams, initiation of the most effective secondary prevention strategy at the time of hospital discharge will help to ensure optimal long-term management of patients after an atherothrombotic event.

    View details for PubMedID 19179811

  • The unique biology of lymphatic edema. Lymphatic research and biology Rockson, S. G. 2009; 7 (2): 97-100

    Abstract

    Sadly, the subject of lymphatic vascular insufficiency continues to engender relative neglect by health care professionals, which represents a source of frustration and fear among patients. A re-consideration of the unique, complex biology of lymphatic vascular disorders has the capacity both to reinvigorate interest and facilitate the implementation of the correct, existing treatment interventions for individuals affected by these disease states. While most of this complex lymphatic biology remains somewhat elusive, growing insights into the molecular mechanisms of lymphatic development and repair have been instructive. Present and future considerations in lymphedema diagnosis and management must acknowledge the unique tissue biology of this disorder. Many changes are unique to the lymphatic mechanisms of chronic edema. The profound stimulus to collagen deposition in the integument seems to be unique to chronic lymphatic edema, although this biology remains largely unexplicated. Several lines of evidence also suggest that lymphatic function has a unique and important influence upon adipose biology. Molecular investigation of murine models of human acquired lymphedema are beginning to shed light on these processes. Such focused mechanistic, approaches to the study of lymphedema and other lymphatic diseases are vital, as we attempt to expand our insights into the complex biology of lymphedema and its potential responsiveness to pharmacologic control and molecular intervention, prevention, and reversal.

    View details for DOI 10.1089/lrb.2009.7202

    View details for PubMedID 19522679

  • The lymphatic continuum revisited - Preface LYMPHATIC CONTINUUM REVISITED Rockson, S. G. 2008; 1131: IX-X

    View details for DOI 10.1196/annals.1413.000

    View details for PubMedID 18519954

  • Gorham's disease - An osseous disease of lymphangiogenesis? LYMPHATIC CONTINUUM REVISITED Radhakrishnan, K., Rockson, S. G. 2008; 1131: 203-205

    Abstract

    Gorham's disease, also known as massive osteolysis, Gorham-Stout disease, vanishing bone disease, or, phantom bone disease is a rare disorder of the musculoskeletal system. The disease is characterized by osteolysis in bony segments, with localized proliferation of lymphatic channels. The presence of abundant, leaky systemic lymphatic vessels is often accompanied by chylous ascites. There is no standardized treatment available for Gorham's disease, and its molecular mechanisms remain unclear. Future strategies for understanding Gorham's disease should emphasize its apparent identity as a disease of disordered lymphangiogenesis. Breakthroughs in lymphatic research have identified several lymphangiogenic pathways that may play a relevant role in Gorham's disease.

    View details for DOI 10.1196/annals.1413.022

    View details for PubMedID 18519972

  • Molecular targets for therapeutic lymphangiogenesis in lymphatic dysfunction and disease. Lymphatic research and biology Nakamura, K., Rockson, S. G. 2008; 6 (3-4): 181-189

    Abstract

    The convergence of multiple disciplines upon the study of the lymphatic vasculature has invigorated a renaissance of research, using powerful investigative tools and an exponential growth of interest in this historically underappreciated system. Fundamental discoveries in lymphatic development have yielded relevant animal models for vexing clinical diseases that suffer from nonexistent of minimally effective treatments. Inherited and acquired lymphedema represent the current crux of research efforts to identify potential molecular therapies born from these early discoveries. The importance of the lymphatic system is, however, not limited to lymphedema but encompasses a diverse spectrum of human disease including inflammation and cancer metastasis. As the lymphatic vasculature continues to benefit from fruits of biomedical investigation, translation of mechanistic insights into targeted, rationally-conceived therapeutics will be become a reality.

    View details for DOI 10.1089/lrb.2008.63404

    View details for PubMedID 19093791

  • Reinforcing a continuum of care: In-hospital initiation of long-term secondary prevention following acute coronary syndromes CARDIOVASCULAR DRUGS AND THERAPY Rockson, S. G., DeGoma, E. M., Fonarow, G. C. 2007; 21 (5): 375-388

    Abstract

    Patients with a history of acute coronary syndrome are particularly susceptible to further vascular or ischemic events. Effective secondary prevention following acute coronary syndrome requires multiple medications targeting the different mechanisms of atherothrombosis. The 2002 American College of Cardiology/American Heart Association guidelines for the management of unstable angina and non ST-segment myocardial infarction and the 2004 guidelines for ST-segment myocardial infarction assign priority to the long-term administration of four critical classes of drugs: antiplatelet agents, in particular aspirin and clopidogrel, beta-blockers, angiotensin-converting enzyme inhibitors, and statins.Despite clinical trial evidence demonstrating their ability to reduce cardiovascular morbidity and mortality, available preventive pharmacotherapies remain underutilized. Suboptimal compliance with current recommendations, as with other management guidelines, arises from a host of entrenched physician, patient, and system-related factors. Optimal management of acute coronary syndrome acknowledges a continuum of care in which acute stabilization represents a single important component. Early, in-hospital implementation of secondary preventive measures reinforces the continuum of care approach, promoting a successful transition from treatment to prevention, inpatient to outpatient management, and, when appropriate, subspecialist to generalist care.

    View details for DOI 10.1007/s10557-007-6043-1

    View details for PubMedID 17701334

  • A novel VEGFR3 mutation causes Milroy disease AMERICAN JOURNAL OF MEDICAL GENETICS PART A Butler, M. G., Dagenais, S. L., Rockson, S. G., Glover, T. W. 2007; 143A (11): 1212-1217

    Abstract

    Milroy disease, also known as primary congenital lymphedema, is a hereditary form of lymphedema with autosomal dominant inheritance. Individuals with Milroy disease are typically characterized by congenital onset of lymphedema of the lower limbs due to hypoplasia of the lymphatic vessels. The genetic basis of most cases of Milroy disease has not been established, although mutations in the vascular endothelial growth factor receptor VEGFR3 (FLT-4) are responsible for some cases with 17 mutations described to date. In this report, we describe a novel VEGFR3 mutation in exon 22 in a four-generation family in which congenital lymphedema segregates in an autosomal dominant manner. In addition to lymphedema, affected family members had other clinical manifestations associated with Milroy disease including hydrocele, ski jump toenails, large caliber veins, and subcutaneous thickening. We screened VEGFR3 for mutations which revealed a novel 3059A>T transversion in exon 22 resulting in Q1020L missense mutation in the second tyrosine kinase domain of VEGFR3. This mutant allele segregated with lymphedema among affected individuals with incomplete penetrance. This is the first report of an exon 22 mutation in Milroy disease.

    View details for DOI 10.1002/ajmg.a.31703

    View details for Web of Science ID 000246955700012

    View details for PubMedID 17458866

  • Rapid diagnosis of myocardial injury with troponin T and CK-MB relative index MOLECULAR DIAGNOSIS & THERAPY Engel, G., Rockson, S. G. 2007; 11 (2): 109-116

    Abstract

    Current hospital practice involves protracted observation of chest-pain patients to rule out myocardial infarction. Concurrent measurement of multiple biomarkers may increase sensitivity and make rapid diagnosis feasible.We sought to determine the optimal biomarker strategy for highly sensitive, early diagnosis of myocardial injury.A prospective evaluation of 171 acute coronary syndrome patients admitted to a single university medical center was performed. Blood tests for creatine kinase (CK), CK myocardial band isoenzyme (CK-MB), and troponin T were obtained at 0, 3, 6, 8, and 16 hours after presentation to the emergency department. Myocardial injury was defined as a troponin T level of >or=0.03 ng/mL.Troponin T had sensitivities of 79.7%, 95.7%, and 98.4% at the time of initial presentation, 3 and 6 hours after presentation, respectively. Using a combination of troponin T and CK-MB relative index, sensitivity on presentation was increased to 90.6%. The sensitivity was improved to 97.9% and 100% at 3 and 6 hours, respectively.This study demonstrates that the diagnosis of myocardial injury can be accurately excluded within 6 hours of admission with high sensitivity using troponin T. The combination of troponin T and CK-MB relative index provided the largest improvement in diagnostic sensitivity at patient arrival. These results support the feasibility of rapid, efficient triage for the emergent presentation of patients with chest pain.

    View details for PubMedID 17397247

  • Biomarkers of lymphatic function and disease MOLECULAR DIAGNOSIS & THERAPY Nakaniura, K., Rockson, S. G. 2007; 11 (4): 227-238

    Abstract

    Substantial advances have accrued over the last decade in the identification of the processes that contribute to lymphatic vascular development in health and disease. Identification of distinct regulatory milestones, from a variety of genetic models, has led to a stepwise chronology of lymphatic development. Several molecular species have been identified as important tissue biomarkers of lymphatic development and function. At present, vascular endothelial growth-factor receptor (VEGFR)-3/VEGF-C/VEGF-D signaling has proven useful in the identification of clinical lymphatic metastatic potential and the assessment of cancer prognosis. Similar biomarkers, to be utilized as surrogates for the assessment of inherited and acquired diseases of the lymphatic circulation, are actively sought, and will represent a signal advance in biomedical investigation.

    View details for Web of Science ID 000249349200003

  • Lymphedema. Current treatment options in cardiovascular medicine Rockson, S. G. 2006; 8 (2): 129-136

    Abstract

    Aggressively applied decongestive measures (ie, manual lymphatic drainage, low-stretch bandaging, exercise, skin care, application of compressive elastic garments) are the mainstay of lymphatic therapy. Therapeutic regimens should differentiate between the sequential goals of acute volume reduction and maintenance of limb volume. Elastic garments should not be employed until maximal volume reduction has been attained through decongestive lymphatic techniques. It is my opinion that use of intermittent pneumatic compression devices can play an important adjunctive role to decongestive lymphatic therapy but should not be substituted for these techniques. At this time, I am not inclined to use pharmacologic therapy in these patients but anxiously await the results of studies that might demonstrate efficacy for molecular approaches. Surgical intervention is reserved for a small number of well-selected patients. Liposuction for volume reduction appears to be a very promising approach for specific patients.

    View details for PubMedID 16533487

  • Literature watch. Lymphatic research and biology Rockson, S. G. 2006; 4 (1): 57-61

    View details for PubMedID 16569210

  • Addressing the unmet needs in lymphedema risk management. Lymphatic research and biology Rockson, S. G. 2006; 4 (1): 42-46

    View details for PubMedID 16569207

  • The lymphatic continuum continues. Lymphatic research and biology Rockson, S. G. 2006; 4 (1): 1-2

    View details for PubMedID 16569199

  • Indirect magnetic resonance lymphangiography to assess lymphatic function in experimental murine lymphedema. Lymphatic research and biology Pan, D., Suzuki, Y., Yang, P. C., Rockson, S. G. 2006; 4 (4): 211-216

    Abstract

    Recently, indirect magnetic resonance lymphangiography with gadolinium (Gd) has been demonstrated to offer the potential for safe, high-resolution visualization of the lymphatic vessels, in addition to the lymph nodes. In this study, the potential utility of indirect Gd contrast magnetic resonance imaging of lymphatic vascular function was investigated in the murine tail. Functional imaging of healthy mice is contrasted with the findings in experimentally-induced lymphatic vascular insufficiency.Postsurgical lymphedema was experimentally created in the murine tail. Normal and lymphedematous mouse tails were imaged following direct subcutaneous administration of Gadolinium-DTPA, 0.1 mmol/kg. Images were obtained in axial and coronal planes with a T1-weighted spin echo inversion-recovery sequence.In the normal tail, both of the bilateral major collecting lymphatics were clearly visualized as the Gd tracer was cleared from the interstitial compartment. In contrast, the Gd tracer accumulated at the prior surgical site in the lymphedematous tail. Quantitative assessment of Gd clearance demonstrates that accumulation of Gd correlates with the impedance to lymph flow proximal to the site of surgical lymphatic ablation.Magnetic resonance is a feasible and reliable method to be applied to quantitative functional imaging of the lymphatic vasculature in experimental models of lymphedema.

    View details for PubMedID 17394404

  • Treprostinil for the treatment of severe digital necrosis in systemic sclerosis VASCULAR MEDICINE Engel, G., Rockson, S. G. 2005; 10 (1): 29-32

    Abstract

    We report a case of severe digital ulcerations associated with systemic sclerosis, successfully treated with treprostinil (Remodulin). There was improvement within days of the treatment initiation; complete healing was accomplished after 16 weeks of therapy. Patients with systemic sclerosis and peripheral small vessel disease have limited therapeutic options. Treprostinil is a prostacyclin analogue that can be delivered by subcutaneous infusion and is approved in the USA only for treatment of primary pulmonary hypertension. This report provides an impressive example of an alternative, complementary indication for the use of treprostinil.

    View details for DOI 10.1191/1358863x05vm579cr

    View details for PubMedID 15920997

  • Therapeutics for lymphatic disease: the role of the pharmaceutical and biotechnology sector. Lymphatic research and biology Rockson, S. G. 2005; 3 (3): 103-104

    View details for PubMedID 16190814

  • The lymphatic biology of Kaposi's sarcoma. Lymphatic research and biology Cheung, L., Rockson, S. G. 2005; 3 (1): 25-35

    View details for PubMedID 15770083

  • Lymphedema therapy in the vascular anomaly patient: therapeutics for the forgotten circulation. Lymphatic research and biology Rockson, S. G. 2005; 3 (4): 253-255

    View details for PubMedID 16379595

  • Literature watch. A genetic Xenopus laevis tadpole model to study lymphangiogenesis. Lymphatic research and biology Rockson, S. G. 2005; 3 (4): 263-267

    View details for PubMedID 16379598

  • Benefits of resident work hours regulation ANNALS OF INTERNAL MEDICINE Skeff, K. M., Ezeji-Okoye, S., Pompei, P., Rockson, S. 2004; 140 (10): 816-817

    View details for PubMedID 15148069

  • The effect of VEGF-C-induced lymphangiogenesis on gene expression profiles in experimental lymphedema 5th Annual Conference on Arteriosclerosis, Thrombosis, and Vascular Biology Kiazand, A., Tsao, P., An, A. C., Han, J., Swanson, J., Berkowski, A., Karkkainen, M., Alitalo, K., Rockson, S. G. LIPPINCOTT WILLIAMS & WILKINS. 2004: E62–E62
  • The effect of VEGF-C-Induced Lymphangiogenesis on Expression profiles for Lymphangiogenesis-related genes in experimental lymphedema Experimental Biology 2004 Annual Meeting Kiazand, A., Berkowski, J. A., An, A. C., Swanson, J., Han, J., Tsao, P., Alitalo, K., Karkkainen, M., Rockson, S. G. FEDERATION AMER SOC EXP BIOL. 2004: A635–A635
  • Comparing the guidelines: Anticoagulation therapy to optimize stroke prevention in patients with atrial fibrillation JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY Rockson, S. G., Albers, G. W. 2004; 43 (6): 929-935

    Abstract

    Atrial fibrillation (AF) is an important risk factor for stroke. According to a pooled analysis of controlled clinical trials with warfarin, anticoagulation therapy reduces stroke risk by 62%. However, clinicians must decide whether the benefit of long-term anticoagulation therapy with available agents outweighs the risk of bleeding for individual patients. Guidelines issued by the American College of Chest Physicians and by the joint American College of Cardiology, American Heart Association, and the European Society of Cardiology task force recommend antithrombotic therapy to protect AF patients from stroke based on risk-stratification algorithms. Risk factors for stroke AF patients include age > or =75 years; hypertension; thyrotoxicosis; diabetes; cardiovascular disease; congestive heart failure; and history of stroke, transient ischemic attack, or thromboembolism. Patients at high risk for stroke experience greater absolute benefit from anticoagulation therapy than patients at low risk. The guidelines are consistent in recommendations for high-risk patients (warfarin therapy, international normalized ratio 2.0 to 3.0) and low-risk patients (aspirin 325 mg), but differ for intermediate-risk patients with diabetes or heart disease. The guidelines continue to evolve, and future guidelines are likely to incorporate new clinical data, including the CHADS(2) algorithm for determining risk and the results of the Atrial Fibrillation Follow-up Investigation of Rhythm Management trial, the Rate Control versus Electrical Cardioversion for Persistent Atrial Fibrillation study, and the Stroke Prevention Using an Oral Thrombin Inhibitor in Atrial Fibrillation II to V trials.

    View details for DOI 10.1016/j.jacc.2003.11.028

    View details for PubMedID 15028346

  • Lymphatic biology and disease: is it being taught? Who is listening? Lymphatic research and biology Rockson, S. G., Granger, D. N., Skeff, K. M., Chaite, W. 2004; 2 (2): 86-95

    View details for PubMedID 15615490

  • The elusive adipose connection. Lymphatic research and biology Rockson, S. G. 2004; 2 (3): 105-106

    View details for PubMedID 15609810

  • Tumors, wounds, and lymph. Lymphatic research and biology Rockson, S. G. 2004; 2 (4): 153-154

    View details for PubMedID 15650384

  • How can lymphatic research influence lymphatic education? Lymphatic research and biology Rockson, S. G. 2004; 2 (2): 67-68

    View details for PubMedID 15615487

  • The potential for molecular treatment strategies in lymphatic disease. Lymphatic research and biology An, A., Rockson, S. G. 2004; 2 (4): 173-181

    View details for PubMedID 15650387

  • Coronary restenosis: A review of mechanisms and management AMERICAN JOURNAL OF MEDICINE Rajagopal, V., Rockson, S. G. 2003; 115 (7): 547-553

    Abstract

    Percutaneous coronary interventions represent an attractive alternative to surgical revascularization; nevertheless, these techniques continue to be characterized by their propensity to elicit restenosis. Despite an exhaustive search for an effective pharmacotherapy to treat or prevent restenosis, hundreds of clinical trials have failed to identify an agent with proven therapeutic benefit. Recently, however, the Food and Drug Administration approved intracoronary radiation (brachytherapy) as a viable therapeutic option for in-stent stenosis. In addition, recent randomized trials have shown encouraging results for drug-eluting stents. This article reviews the pathophysiology of restenosis, along with current and future treatment options.

    View details for DOI 10.1016/S0002-9343(03)00477-7

    View details for PubMedID 14599634

  • Endothelial cell diversity revealed by global expression profiling PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA Chi, J. T., Chang, H. Y., Haraldsen, G., Jahnsen, F. L., Troyanskaya, O. G., Chang, D. S., Wang, Z., Rockson, S. G., van de Rijn, M., Botstein, D., Brown, P. O. 2003; 100 (19): 10623-10628

    Abstract

    The vascular system is locally specialized to accommodate widely varying blood flow and pressure and the distinct needs of individual tissues. The endothelial cells (ECs) that line the lumens of blood and lymphatic vessels play an integral role in the regional specialization of vascular structure and physiology. However, our understanding of EC diversity is limited. To explore EC specialization on a global scale, we used DNA microarrays to determine the expression profile of 53 cultured ECs. We found that ECs from different blood vessels and microvascular ECs from different tissues have distinct and characteristic gene expression profiles. Pervasive differences in gene expression patterns distinguish the ECs of large vessels from microvascular ECs. We identified groups of genes characteristic of arterial and venous endothelium. Hey2, the human homologue of the zebrafish gene gridlock, was selectively expressed in arterial ECs and induced the expression of several arterial-specific genes. Several genes critical in the establishment of left/right asymmetry were expressed preferentially in venous ECs, suggesting coordination between vascular differentiation and body plan development. Tissue-specific expression patterns in different tissue microvascular ECs suggest they are distinct differentiated cell types that play roles in the local physiology of their respective organs and tissues.

    View details for DOI 10.1073/pnas.1434429100

    View details for PubMedID 12963823

  • Endothelial dysfunction: Clinical strategies for treating oxidant stress AMERICAN HEART JOURNAL Fenster, B. E., Tsao, P. S., Rockson, S. G. 2003; 146 (2): 218-226

    Abstract

    A growing body of evidence has demonstrated that oxidants play a critical role in the pathogenesis of endothelial dysfunction. Pathologic processes fundamental to development and progression of endothelial dysfunction such as the oxidation of LDL, the loss of bioavailable nitric oxide, and the vascular inflammatory response are all modulated by oxidant stress. Therapeutic strategies to reverse endothelial dysfunction have begun to focus on agents with the ability to ameliorate oxidant stress.Preclinical and clinical studies evaluating the actions of antioxidants as well as traditional cardiovascular therapies in ameliorating oxidative stress and endothelial dysfunction were reviewed through the use of a MEDLINE search of English language articles published between the years of 1992 and 2002.Antioxidants appear to be an attractive candidate therapy, yet despite compelling preclinical evidence supporting their benefits, efforts to validate the use of vitamins C and E in a clinical setting have been conflicting. In contrast, conventional cardiovascular therapies such as ACE inhibitors, statins, insulin-sensitizing agents, and estrogens have been shown to alleviate endothelial dysfunction, often independent of their effects on systemic disease processes.These agents restore endothelial function through their salutary effects on pathologic vascular oxidative processes.

    View details for DOI 10.1016/S0002-8703(03)00087-X

    View details for PubMedID 12891188

  • Poor early sensitivity of myoglobin for the diagnosis of myocardial injury Asia Pacific Scientific Forum on New Discoveries in Cardiovascular Disease and Stroke Engel, G., Rockson, S. G. LIPPINCOTT WILLIAMS & WILKINS. 2003: E144–E144
  • Lymphangiogenesis in lymphatic insufficiency: Lymphatic endothelial and inflammatory RNA expression patterns 4th Annual Conference on Arteriosclerosis Thrombosis and Vascular Biology Shin, W. S., Rockson, N. B., Sanchez, D. R., Midde, R., Alitalo, K., Karkkainen, M., Tsao, P. S., Rockson, S. G. LIPPINCOTT WILLIAMS & WILKINS. 2003: A52–A52
  • The third circulation: Radionuclide lymphoscintigraphy in the evaluation of lymphedema JOURNAL OF NUCLEAR MEDICINE Szuba, A., Shin, W. S., Strauss, H. W., Rockson, S. 2003; 44 (1): 43-57

    Abstract

    Lymphedema-edema that results from chronic lymphatic insufficiency-is a chronic debilitating disease that is frequently misdiagnosed, treated too late, or not treated at all. There are, however, effective therapies for lymphedema that can be implemented, particularly after the disorder is properly diagnosed and characterized with lymphoscintigraphy. On the basis of the lymphoscintigraphic image pattern, it is often possible to determine whether the limb swelling is due to lymphedema and, if so, whether compression garments, massage, or surgery is indicated. Effective use of lymphoscintigraphy to plan therapy requires an understanding of the pathophysiology of lymphedema and the influence of technical factors such as selection of the radiopharmaceutical, imaging times after injection, and patient activity after injection on the images. In addition to reviewing the anatomy and physiology of the lymphatic system, we review physiologic principles of lymphatic imaging with lymphoscintigraphy, discuss different qualitative and quantitative lymphoscintigraphic techniques and their clinical applications, and present clinical cases depicting typical lymphoscintigraphic findings.

    View details for PubMedID 12515876

  • Immune traffic: a functional overview. Lymphatic research and biology Beilhack, A., Rockson, S. G. 2003; 1 (3): 219-234

    Abstract

    The efficient function of the immune system necessitates the complex interaction of antigens, antigen-presenting cells, and cell populations that modulate, regulate and effectuate the immune response. In order to overcome the spatial limitations that are imposed by the constraints of the system, the immune system has evolved a dependence upon the lymphatic vasculature to serve the biological needs of immune trafficking. This review will focus upon useful ex vivo and intact animal models that possess the ability to provide valuable information about leukocyte trafficking.

    View details for PubMedID 15624439

  • Animal models for the study of lymphatic insufficiency. Lymphatic research and biology Shin, W. S., Szuba, A., Rockson, S. G. 2003; 1 (2): 159-169

    Abstract

    Lymphedema is the term commonly employed to describe the spectrum of pathological states that arise as a consequence of functional lymphatic insufficiency. These human disease entities currently lack an effective cure. Satisfactory therapeutic strategies for both primary and secondary lymphedema will require additional insight into the complex cellular mechanisms and responses that comprise both normal lymphatic function and its regional derangement in states of pathologic dysfunction. Such insights must, initially, be derived from suitable animal models of the chronic human disease process. Historically, efforts to replicate the untreated disease of human lymphedema in animals, through surgery, irradiation, and toxicology, have been fraught with difficulty. The major impediments to the creation of satisfactory animal models have included an inability to reproduce the chronic disease in a stable, reproducible format. Recently, with the promise of potentially successful growth factor-mediated therapeutic lymphangiogenesis, and with the enhanced availability of investigative tools to assess therapeutic responses to molecular therapies, there has been a resurgence of interest in the development of viable animal models of lymphatic insufficiency. Current research has led to the development of genetic and postsurgical models of lymphedema that closely simulate the human conditions of primary and secondary lymphatic insufficiency, respectively. Such models will help to refine the assessment of various therapeutic approaches and their potential applicability to human disease interventions.

    View details for PubMedID 15624423

  • Quantitative radionuclide lymphoscintigraphy predicts outcome of manual lymphatic therapy in breast cancer-related lymphedema of the upper extremity NUCLEAR MEDICINE COMMUNICATIONS Szuba, A., Strauss, W., Sirsikar, S. P., Rockson, S. G. 2002; 23 (12): 1171-1175

    Abstract

    Secondary lymphedema is a localized, acquired lymphatic microcirculatory disturbance that affects large numbers of patients after breast cancer therapy. There is a paucity of objective methods to quantitate lymphatic function and to anticipate the response to therapeutic interventions. We applied radionuclide lymphoscintigraphy to evaluate lymphatic transport and axillary lymph node visualization in women following breast cancer therapy to determine the utility of these data in these patients. Lymphoscintigraphy was performed after subcutaneous injection of 0.25 mCi of Tc-filtered sulfur colloid. Subcutaneous accumulation of radiotracer ('dermal backflow') and the visualization of axillary lymph nodes were graded using our own scoring system. The ratio of radioactivity within the affected to normal axillae (ARR) was also quantified. Nineteen patients with lymphedema after breast cancer therapy were evaluated. The disease severity was documented by serial measurements of the limb volume using the truncated cone formula. Responses to therapy were quantified after completion of the therapy. There was a correlation between the ARR and the percentage reduction in edema volume. The lymphoscintigraphic score correlated with the initial arm volume excess and with the durationof lymphedema. It can be concluded that quantitative and semi-quantitative assessment by radionuclide lymphoscintigraphy represents a potentially useful tool for the clinical assessment of upper extremity lymphedema.

    View details for DOI 10.1097/01.mnm.0000046208.83338.da

    View details for Web of Science ID 000180086600004

    View details for PubMedID 12464781

  • Decongestive lymphatic therapy for patients with breast carcinoma-associated lymphedema - A randomized, prospective study of a role for adjunctive intermittent pneumatic compression CANCER Szuba, A., Achalu, R., Rockson, S. G. 2002; 95 (11): 2260-2267

    Abstract

    Disruption of the lymphatic circulation through breast carcinoma-associated axillary lymph node dissection, with or without radiation therapy, reportedly is the most common cause of lymphedema in developed countries. There is no cure for breast carcinoma-associated lymphedema. Although intermittent pneumatic compression (IPC) has been acknowledged as a potential component of the multidisciplinary therapeutic strategy in the treatment of patients with breast carcinoma-associated lymphedema, prospective study of its adjunctive safety and efficacy is required.IPC was assessed as a component of the initial therapeutic regimen for newly treated patients with breast carcinoma-associated lymphedema. Twenty-three patients who had not previously been treated for lymphedema were randomized to receive either decongestive lymphatic therapy (DLT) alone or DLT with daily adjunctive IPC. Patients with stable, treated, breast carcinoma-associated lymphedema also were assessed in the maintenance phase of therapy. Twenty-seven patients were randomized either to DLT alone or to DLT coupled with daily IPC. In both studies, objective assessment included serial measurement of volume by water displacement, tissue tonometry to assess elasticity of the skin, and goniometry to measure joint mobility.During initial treatment, the addition of IPC to standard DLT yielded an additional mean volume reduction (45.3% vs. 26%; P < 0.05). During maintenance DLT alone, there was a mean increase in volume (32.7 +/- 115.2 mL); with DLT and IPC, there was a mean volume reduction (89.5 +/- 195.5 mL; P < 0.05). In both studies, IPC was tolerated well without detectable adverse effects on skin elasticity or joint range of motion.When IPC is used adjunctively with other, established elements of DLT, it provides an enhancement of the therapeutic response. IPC is well tolerated and remarkably free of complications.

    View details for DOI 10.1002/cncr.10976

    View details for PubMedID 12436430

  • Rapid diagnosis of myocardial injury with troponin T and CK-MB relative index American-Heart-Association Abstracts From Scientific Sessions Engel, G., Rockson, S. G. LIPPINCOTT WILLIAMS & WILKINS. 2002: 531–31
  • Lymphedema-lymphangiectasia-mental retardation (Hennekam) syndrome: A review AMERICAN JOURNAL OF MEDICAL GENETICS Van Balkom, I. D., Alders, M., Allanson, J., Bellini, C., Frank, U., de Jong, G., Kolbe, I., Lacombe, D., Rockson, S., Rowe, P., Wijburg, F., Hennekam, R. C. 2002; 112 (4): 412-421

    Abstract

    The Hennekam syndrome is an infrequently reported heritable entity characterized by lymphedema, lymphangiectasia, and developmental delay. Here we add an additional 8 patients, and compare their findings to the 16 cases from the literature. The lymphedema is usually congenital, can be markedly asymmetrical, and, often, gradually progressive. Complications such as erysipelas are common. The lymphangiectasias are present in the intestines, but have also been found in the pleura, pericardium, thyroid gland, and kidney. Several patients have demonstrated congenital cardiac and blood vessel anomalies, pointing to a disturbance of angiogenesis in at least some of the patients. Facial features are variable, and are chiefly characterized, in a typical patient, by a flat face, flat and broad nasal bridge, and hypertelorism. Facial features are thought to mirror the extent of intrauterine facial lymphedema, or may be caused by lymphatic obstruction that affects the early migration of neural crest tissue. Other anomalies have included glaucoma, dental anomalies, hearing loss, and renal anomalies. The psychomotor development varies widely, even within a single family, from almost normal development to severe mental retardation. Convulsions are common. The existence of 10 familial cases, equal sex ratio, increased parental consanguinity rate (4/20 families), and absence of vertical transmission are consistent with an autosomal recessive pattern of inheritance. It seems likely that most (but not all) manifestations of the entity can be explained as sequences of impaired prenatal and postnatal lymphatic flow, suggesting that the causative gene(s) should have a major function in lymphangiogenesis.

    View details for DOI 10.1002/ajmg.10707

    View details for Web of Science ID 000178568700018

    View details for PubMedID 12376947

  • Myocarditis in systemic lupus erythematosus AMERICAN JOURNAL OF MEDICINE Wijetunga, M., Rockson, S. 2002; 113 (5): 419-423

    Abstract

    Although clinical manifestations of myocarditis in systemic lupus erythematosus are uncommon, noninvasive cardiac testing may detect subclinical cases. The pathogenesis of myocarditis in systemic lupus erythematosus has been ascribed to many factors, including autoimmunity, medications, and coexisting diseases. Lupus myocarditis merits urgent clinical attention because of the likely progression to arrhythmias, conduction disturbances and heart block, dilated cardiomyopathy, and heart failure. Endomyocardial biopsy can be used to identify the underlying inflammatory histopathology. Usual therapy includes high-dose corticosteroids, in addition to standard cardiac medications.

    View details for Web of Science ID 000178799400009

    View details for PubMedID 12401537

  • Diagnosis and treatment of concomitant venous obstruction in patients with secondary lymphedema JOURNAL OF VASCULAR AND INTERVENTIONAL RADIOLOGY Szuba, A., Razavi, M., Rockson, S. G. 2002; 13 (8): 799-803

    Abstract

    It has been proposed that concomitant iatrogenic venous obstruction substantially contributes to the appearance and severity of the secondary lymphedema that follows cancer surgery, radiation, and other traumas. The purpose of this study was to investigate the frequency of venous obstruction in the clinical presentation of patients with secondary lymphedema and to analyze the efficacy of interventional therapy in this patient population.The experience of the university center for lymphatic and venous disorders with combined lymphaticovenous edema was retrospectively examined. The records and clinical course were reviewed for all patients referred to a university lymphedema center for evaluation between January 1996 and March 1999. During this interval, in 365 patients with lymphedema, 35 radiocontrast venograms were obtained to evaluate the suspected presence of mixed lymphaticovenous edema. Venographic evidence of venous stenosis (>50%) or occlusion was analyzed, as were the technical success of the intervention, determined by ability to cross the affected segment of the vein and perform venoplasty and place the stent, and the clinical success of the intervention assessed by relief of clinical symptoms (edema, pain) within 24 hours.The diagnosis of venous obstruction was confirmed in 17 patients (4.6% of all patients with lymphedema; 49% of patients studied with venography). Venography disclosed clinically relevant venous stenosis in five of seven patients with edema of the upper extremity and in six of 10 patients with leg lymphedema. Venous occlusion was found in two of seven patients with upper extremity edema and in four of 10 patients with leg lymphedema. Percutaneous endovascular venoplasty was attempted in all 17 patients and was successful in 16. Subsequent venous stent placement was performed in three patients with upper extremity edema and in all patients with lower extremity lymphedema. Clinical amelioration of edema was observed in 15 of these 17 patients. Amelioration was assessed by relief of symptoms, improvement in function, and reduction in limb girth.This study supports the clinical importance of concomitant venous obstruction in some patients with chronic secondary lymphedema. Edema can often be ameliorated through percutaneous catheter-based interventions.

    View details for PubMedID 12171983

  • Therapeutic lymphangiogenesis in a rabbit ear model of chronic post-surgical lymphatic insufficiency Szuba, A., Skobe, M., Shin, W., Beynet, D. P., Rockson, N. B., Dakhil, N., Goris, M. L., Strauss, H. W., Quertermous, T., Alitalo, K., Rockson, S. G. FEDERATION AMER SOC EXP BIOL. 2002: A516–A516
  • A model for chronic, post-surgical lymphatic insufficiency Shin, W., Szuba, A., Skobe, M., Beynet, D. P., Rockson, N. B., Dakhil, N., Goris, M. L., Strauss, H. W., Quertermous, T., Alitalo, K., Rockson, S. G. FEDERATION AMER SOC EXP BIOL. 2002: A123–A124
  • A model of acute, post-surgical lymphedema Beynet, D. P., Szuba, A., Skobe, M., Rockson, N. B., Dakhil, N., Shin, W., Goris, M. L., Strauss, H. W., Quertermous, T., Alitalo, K., Rockson, S. G. FEDERATION AMER SOC EXP BIOL. 2002: A124–A124
  • Preclinical models of lymphatic disease - The potential for growth factor and gene therapy Conference on the Lymphatic Continuum Rockson, S. G. NEW YORK ACAD SCIENCES. 2002: 64–75

    Abstract

    The human disease states that are characterized by functional lymphatic insufficiency currently lack a cure. Molecular approaches may ultimately provide a therapeutic window to reverse the stigmata of both primary and secondary lymphatic insufficiency. To harness the potential therapeutic power of lymphangiogenesis, testing the safety and efficacy of the treatment response will be necessary. This, in turn, necessitates the availability of suitable preclinical animal models of the disease processes in question, along with suitable research tools to permit an assessment of the response to applied therapies. An ideal model would reproducibly and inexpensively replicate the untreated disease of human lymphedema. It would closely simulate the biology, as we understand it, of the human disease, and would replicate both the pathogenesis of the disease, including its natural history and the temporal patterns of its clinical expression. In this way, one might aspire to make valid predictions about the human applicability of therapy by extrapolation from observations in animal models. In addition to the availability of suitable animal models, the required investigative tools must also be available. In the context of lymphangiogenesis, to assess the therapeutic response, one must certainly possess the ability to recognize newly developed lymphatic vasculature. Sophisticated immunohistochemical and imaging techniques make this increasingly feasible. Initial experimental observations indicate that growth factor and gene therapy with VEGF-C holds promise for the treatment of both primary and secondary forms of lymphedema.

    View details for PubMedID 12543717

  • Lymphedema after surgery for cancer - The role of patient support groups in patient therapy DISEASE MANAGEMENT & HEALTH OUTCOMES Rockson, S. G. 2002; 10 (6): 345-347
  • New tools for lymphatic investigation - Panel discussion Conference on the Lymphatic Continuum Rockson, S. G., Niklason, L., Zawieja, D., Ochoa, E., Granger, Gannon, B., WILTING, J., Simonian, S., Olszewski, W., Hayward NEW YORK ACAD SCIENCES. 2002: 35–38
  • Biological principles - Panel discussion Conference on the Lymphatic Continuum Rockson, Slavin, S., Detmer, M., Miller, A., Mouta, C., Ferrell, Zawiea, Thurston, G., Glover, T. NEW YORK ACAD SCIENCES. 2002: 76–79
  • The lymphatic continuum - The past, present, and exciting future of lymphatic research Conference on the Lymphatic Continuum Rockson, S. G. NEW YORK ACAD SCIENCES. 2002: 1–4

    View details for PubMedID 12543710

  • The role of chemokines in human cardiovascular pathology: enhanced biological insights ATHEROSCLEROSIS Shin, W. S., Szuba, A., Rockson, S. G. 2002; 160 (1): 91-102

    Abstract

    A growing body of experimental evidence supports the pivotal role of chemokines in the pathogenesis of vascular disease. The endothelial expression of monocyte chemoattractant protein-1 (MCP-1) is apparently essential for the earliest cellular responses of atherogenesis. Many atherogenic and anti-atherogenic stimuli can be construed to exert their effects predominantly upon MCP-1 expression within the vascular wall. The atherogenic effects of interleukin-8 (IL-8) seem to be mediated through the down-regulation of the tissue inhibitor of metalloproteinase-1 (TIMP-1). Biological expression of these two important vascular chemokines is further modulated by NF-kappaB. The delineation of these molecular forces that drive atherogenesis increasingly underscores the pivotal role of various chemokines. It is anticipated that more precise delineation of these patterns of gene expression will help to identify molecular targets for the prevention and treatment of atherosclerosis.

    View details for PubMedID 11755926

  • Feasibility and reliability of rapid diagnosis of myocardial infarction AMERICAN JOURNAL OF THE MEDICAL SCIENCES Engel, G., Rockson, S. G. 2001; 322 (6): 339-344

    Abstract

    Prevailing hospital practice dictates a protracted phase of observation for patients with chest pain to establish or exclude the diagnosis of myocardial infarction. Early diagnosis of acute myocardial infarction may improve patient care and reduce both complications and hospital costs. A study was performed to investigate the feasibility of early diagnosis of myocardial infarction within the first 9 hours of the hospital stay.The records of all patients admitted with chest pain within one calendar year were analyzed. The timing of creatine kinase-MB (CK-MB) quantification was determined with reference to the initial phlebotomy (time 0). An enzymatic diagnosis of myocardial infarction was assigned if any determination of CK-MB exceeded the upper limit of normal, and the diagnosis of each patient at or before 9 hours (early diagnosis) was compared to the ultimate diagnosis at 14 to 24 hours (final diagnosis) beyond initial assessment.Of the 528 included patients, 523 patients (99.1%) had identical early and final diagnostic outcomes; 5 patients (0.9%) had conflicting results. An early diagnosis of myocardial infarction was assigned to 195 of the 528 patients (36.9%). Of these, 190 achieved the diagnosis within 9 hours (sensitivity 97.4%). The negative predictive value was 98.5%.Standard CK-MB mass measurements within 9 hours of arrival provided an accurate clinical assessment in > 99% of the cases. The high sensitivity and negative predictive values suggest that early diagnosis of myocardial infarction is feasible and reliable.

    View details for Web of Science ID 000172724700006

    View details for PubMedID 11780691

  • Photoangioplasty recount: Clear punch or dimpled chad? Response CIRCULATION Rockson, S. G., Razavi, M., Szuba, A., Filardo, S., Fitzgerald, P., Cooke, J. P., Yousuf, S., Kramer, P., DeVault, A. R., Renschler, M. F., Adelman, D. C. 2001; 104 (11): E55-E56
  • Angiogenesis and the ischaemic heart EUROPEAN HEART JOURNAL Tabibiazar, R., Rockson, S. G. 2001; 22 (11): 903-918

    View details for Web of Science ID 000169334600007

    View details for PubMedID 11428814

  • Formulating clinical strategies for angiotensin antagonism: A review of preclinical and clinical studies AMERICAN JOURNAL OF MEDICINE Tabibiazar, R., Jamali, A. H., Rockson, S. G. 2001; 110 (6): 471-480

    Abstract

    Extensive animal studies and a growing number of human clinical trials have now definitively demonstrated the central role of the renin-angiotensin-aldosterone system in the expression and modulation of cardiovascular disease. In contrast to the original hypothesis, the benefits of angiotensin antagonism do not emanate from the antihypertensive effect alone. Subsequent extensive investigations of angiotensin blockade suggest that the benefits of this approach may also result from the pharmacologic alteration of endothelial cell function and the ensuing changes in the biology of the vasculature. The more recent availability of direct antagonists of the AT(1) angiotensin receptor has introduced an element of doubt into this realm of clinical decision making. The receptor antagonists and the more widely studied converting-enzyme inhibitors share many endpoint attributes. Nevertheless, the partially overlapping mechanisms of action for the two classes of angiotensin antagonists confer distinct pharmacologic properties, including side effect profiles, mechanisms of action, and theoretic salutary effects upon the expression of cardiovascular disease. The current review will attempt to contrast the biology of angiotensin converting-enzyme inhibition with angiotensin II receptor antagonism. A discussion of the differential effects of these drug classes on endothelial cell function and on the modulation of vascular disease will be utilized to provide a theoretic framework for clinical decision making and therapeutics.

    View details for Web of Science ID 000168267700008

    View details for PubMedID 11331059

  • Lymphedema AMERICAN JOURNAL OF MEDICINE Rockson, S. G. 2001; 110 (4): 288-295

    Abstract

    Lymphedema is a set of pathologic conditions that are characterized by the regional accumulation of excessive amounts of interstitial protein-rich fluid. These occur as a result of an imbalance between the demand for lymphatic flow and the capacity of the lymphatic circulation. Lymphedema can result from either primary or acquired (secondary) disorders. In this review, the pathophysiology, classification, natural history, differential diagnosis, and treatment of lymphedema are discussed.

    View details for Web of Science ID 000167190300007

    View details for PubMedID 11239847

  • Photoangioplasty for human peripheral atherosclerosis - Results of a phase I trial of photodynamic therapy with motexafin lutetium (Antrin) 72nd Annual Scientific Session of the American-Heart-Association Rockson, S. G., Kramer, P., Razavi, M., Szuba, A., Filardo, S., Fitzgerald, P., Cooke, J. P., Yousuf, S., DeVault, A. R., Renschler, M. F., Adelman, D. C. LIPPINCOTT WILLIAMS & WILKINS. 2000: 2322–24

    Abstract

    In photoangioplasty, light activation of a photosensitive drug offers the potential for treatment of long segments of vascular disease. This is a brief description of a study designed to evaluate the safety and tolerability of a new photosensitizer, Antrin (motexafin lutetium), in the endovascular treatment of atherosclerosis.An open-label, single-dose, escalating drug- and light-dose study was performed in patients with atherosclerotic peripheral arterial insufficiency. Clinical evaluation, serial quantitative angiography, and intravascular ultrasonography were performed. Therapy was well tolerated, and only minor side effects were observed. Treatment produced no deleterious vascular effects. Although this study was not designed to examine clinical efficacy, several secondary end points suggested a favorable therapeutic effect.This phase I study demonstrates that photoangioplasty with motexafin lutetium is well tolerated and safe. Preliminary efficacy data suggest a future role for the treatment of flow-limiting atherosclerosis.

    View details for Web of Science ID 000165169200001

    View details for PubMedID 11067782

  • Decongestive lymphatic therapy for patients with cancer-related or primary lymphedema AMERICAN JOURNAL OF MEDICINE Szuba, A., Cooke, J. P., Yousuf, S., Rockson, S. G. 2000; 109 (4): 296-300

    Abstract

    A prospective evaluation was undertaken to assess the efficacy of intensive, short-term decongestive lymphatic therapy coupled with focused patient instruction in long-term self-care for the management of lymphedema.The therapeutic responses of 79 patients with lymphedema were analyzed prospectively. Each patient received intensive, short-term decongestive lymphatic therapy, with quantification of the extent and durability of the clinical response. Decongestive lymphatic therapy was performed by therapists trained in these techniques. The mean (+/-SD) duration of therapy was 8+/-3 days. Instruction in self-management techniques was incorporated into the therapeutic regimen by day 3 of the patient's treatment. The mean period of follow-up was 38+/-52 days. Changes in the volume of the affected limb were assessed with a geometric approximation derived from serial measurements of circumference along the axis of the limb.The mean short-term reduction in limb volume was 44%+/-62% of the excess volume in the upper extremities and 42%+/-40% in the lower extremities. At follow-up, these results were adequately sustained: mean long-term excess volume reductions of 38%+/-56% (upper extremities) and 41%+/-27% (lower extremities) were observed.Decongestive lymphatic therapy, combined with long-term self-management, is efficacious in treating patients with lymphedema of the extremity.

    View details for Web of Science ID 000089356600005

    View details for PubMedID 10996580

  • Photoangioplasty - An emerging clinical cardiovascular role for photodynamic therapy CIRCULATION Rockson, S. G., Lorenz, D. P., Cheong, W. F., Woodburn, K. W. 2000; 102 (5): 591-596

    Abstract

    Photodynamic therapy (PDT) has been studied and applied to various disease processes. The potential of PDT for selective destruction of target tissues is especially appealing in cardiovascular disease, in which other existing interventional tools are somewhat nonselective and carry substantial risk of damage to the normal arterial wall. Enthusiasm for photoangioplasty (PDT of vascular de novo atherosclerotic and, potentially, restenotic lesions) is fueled by more effective second-generation photosensitizers and technological advances in endovascular light delivery. This excitement revolves around at least 4 significant attributes of light-activated therapy: the putative selectivity and safety of photoangioplasty, the potential for atraumatic and effective debulking of atheromatous plaque through a biological mechanism, the postulated capability to reduce or inhibit restenosis, and the potential to treat long segments of abnormal vessel by simply using fibers with longer light-emitting regions. The available nonclinical data, coupled with the observations of a new phase I trial in human peripheral atherosclerosis, suggest a promising future for photoangioplasty in the treatment of primary atherosclerosis and prevention of restenosis.

    View details for Web of Science ID 000088486200020

    View details for PubMedID 10920074

  • Lymphedema. Current treatment options in cardiovascular medicine Rockson 2000; 2 (3): 237-242

    Abstract

    Aggressively applied decongestive measures (eg, manual lymphatic drainage, low-stretch bandaging, exercise, skin care, application of compressive elastic garments) are the mainstay of lymphatic therapy. Therapeutic regimens should differentiate between the goals of acute volume reduction and the maintenance of limb volume. Elastic garments should not be employed until maximal volume reduction has been attained through decongestive lymphatic techniques. It is my opinion that use of intermittent pneumatic compression devices can play an important adjunctive role to decongestive lymphatic therapy but should not be substituted for these techniques. At this time, I am not inclined to use pharmacologic therapy in these patients but anxiously await the results of studies that might demonstrate efficacy for molecular approaches. Surgical intervention is reserved for a small number of well-selected patients. Liposuction for volume reduction appears to be a very promising approach for specific patients.

    View details for PubMedID 11096529

  • Benefits of lipid-lowering agents in stroke and coronary heart disease: pharmacoeconomics. Current atherosclerosis reports Rockson, S. G. 2000; 2 (2): 144-150

    Abstract

    Coronary heart disease remains the leading cause of death in the United States. Although coronary heart disease and stroke entail very expensive therapies and extensive hospital utilization, the cost of preventive measures is also quite expensive. In this review, the factors that determine the cost-effectiveness of statin therapy for the primary and secondary prevention of coronary heart disease are discussed. A risk-based strategy for the selection of patients seems to provide cost-effective utilization of this potent treatment strategy. Appropriate patient selection should be accompanied by aggressive measures to improve utilization and compliance through improved physician and patient education.

    View details for PubMedID 11122738

  • Cardiovascular photodynamic therapy: State of the art Conference on Lasers in Surgery - Advanced Characterization, Therapeutics, and Systems X Woodburn, K. W., Rockson, S. G. SPIE-INT SOC OPTICAL ENGINEERING. 2000: 560–68
  • Lymphoscintigraphic manifestations of Hennekam syndrome - A case report ANGIOLOGY Rockson, S. G., De Los Santos, M., Szuba, A. 1999; 50 (12): 1017-1020

    Abstract

    Hennekam syndrome is a rare, recently described genetic disorder in which facial anomalies and mental retardation accompany congenital lymphedema and intestinal lymphangiectasia. Several other somatic abnormalities have variously been described, as have milder degrees of lymphatic dysfunction. The authors herein describe a case of Hennekam syndrome in which the diagnostic difficulties were partially overcome by the judicious use of radionuclide scintigraphy to verify the lymphedematous component of the patient's presentation.

    View details for Web of Science ID 000084362900007

    View details for PubMedID 10609768

  • Complex lower extremity edema in a young woman VASCULAR MEDICINE Rockson, S. G., Szuba, A. 1999; 4 (4): 273-274
  • Lutetium Texaphyrin: A New Therapeutic Tool for Human Atherosclerosis. Current treatment options in cardiovascular medicine Rockson 1999; 1 (3): 199-202

    View details for PubMedID 11096484

  • Fibroblast growth factor as therapy for critical limb ischemia: a case report VASCULAR MEDICINE Cooke, J. P., Bhatnagar, R., Szuba, A., Rockson, S. G. 1999; 4 (2): 89-91

    Abstract

    In an attempt to avert impending, primary amputation, an 85-year-old woman with chronic critical leg ischemia was enrolled in an experimental protocol to induce therapeutic angiogenesis. Treatment consisted of six consecutive, weekly intravenous infusions of recombinant basic fibroblast growth factor (bFGF). Angiographic evaluation was performed before and after therapy. The patient's clinical response was monitored through serial measurements of the ankle/brachial index and by repetitive assessment of limb flow by mercury strain-gauge plethysmography. A beneficial clinical response was detectable by week 4 of therapy, which was characterized by an improved walking distance, relief of ischemic pain, a marked reduction in analgesic consumption, and healing of persistent, unresponsive, painful inflammation of the hallux. The clinical improvement was sustained throughout the remaining weeks of therapy and follow-up evaluation. Plethysmography documented improved blood flow; specifically, the augmentation of digital flow was sustained and correlated with the marked improvement in the patient's clinical status.

    View details for Web of Science ID 000081421600006

    View details for PubMedID 10406455

  • Images in vascular medicine. Complex lower extremity edema in a young woman. Vascular medicine Rockson, S. G., Szuba, A. 1999; 4 (4): 273-274

    View details for PubMedID 10613633

  • Precipitating factors in lymphedema: Myths and realities American-Cancer-Society Workshop on Breast Cancer Treatment-Related Lymphedema Rockson, S. G. JOHN WILEY & SONS INC. 1998: 2814–16

    Abstract

    Lymphedema is an all too common occurrence following breast carcinoma therapy. Despite its prevalence, the predisposing factors to the development of this secondary form of lymphedema remain poorly understood.Several studies have addressed these questions and are reviewed here.Treatment factors that appear to predispose to the late, subjective appearance of lymphedema include the extent of axillary surgery and exposure to high dose axillary radiotherapy, particularly when combined with surgical clearance of the axilla. Other pertinent patient factors may include the presence of hypertension and exposure to airline travel. Clinical features unrelated to the risk of lymphedema development include patient age; drug therapy; time interval to presentation, surgery, or radiotherapy to the breast; total dose of radiation; and menopausal status. The potential importance of concomitant venous abnormalities in these patients is worthy of consideration.Breast carcinoma-related secondary lymphedema is an important subjective and functional problem for affected patients. Additional research into the predisposing factors to this common problem is likely to foster enhanced patient education and to produce more efficacious measures to control this disease.

    View details for Web of Science ID 000077732500008

    View details for PubMedID 9874403

  • Workgroup III - Diagnosis and management of lymphedema American-Cancer-Society Workshop on Breast Cancer Treatment-Related Lymphedema Rockson, S. G., Miller, L. T., Senie, R., Brennan, M. J., Casley-Smith, J. R., Foldi, E., Foldi, M., Gamble, G. L., Kasseroller, R. G., Leduc, A., Lerner, R., Mortimer, P. S., Norman, S. A., Plotkin, C. L., Rinehart-Ayres, M. E., Walder, A. L. JOHN WILEY & SONS INC. 1998: 2882-?
  • American Cancer Society Lymphedema Workshop. Workgroup III: Diagnosis and management of lymphedema. Cancer Rockson, S. G., Miller, L. T., Senie, R., Brennan, M. J., Casley-Smith, J. R., Földi, E., Földi, M., Gamble, G. L., Kasseroller, R. G., Leduc, A., Lerner, R., Mortimer, P. S., Norman, S. A., Plotkin, C. L., Rinehart-Ayres, M. E., Walder, A. L. 1998; 83 (12): 2882-2885

    View details for PubMedID 9874417

  • Photodynamic angioplasty of human atherosclerosis with ANTRIN photosensitization Rockson, S. G., Szuba, A., Razavi, M., Yeung, A. C., Cooke, J. P. LIPPINCOTT WILLIAMS & WILKINS. 1998: 66–66
  • Myocardial ischemia and infarction due to multiple coronary-cameral fistulae: Two case reports and review of the literature CATHETERIZATION AND CARDIOVASCULAR DIAGNOSIS Wolf, A., Rockson, S. G. 1998; 43 (2): 179-183

    Abstract

    The functional significance of coronary-cameral fistulae, and the effect of these arterial anomalies upon effective coronary blood flow, continue to be debated. Two cases of coronary cameral fistulae, each of which illustrates the likelihood of an ischemic substrate, are herein presented, along with a review of the relevant literature regarding this disorder.

    View details for Web of Science ID 000071801100015

    View details for PubMedID 9488552

  • Images in vascular medicine. Phlegmasia coerulea dolens--venous gangrene. Vascular medicine Szuba, A., Cooke, J. P., Rockson, S. G. 1998; 3 (1): 29-31

    View details for PubMedID 9666529

  • Images in vascular medicine. Lymphoscintigraphy in congenital lymphedema. Vascular medicine De Los Santos, M., Szuba, A., Rockson, S. G. 1998; 3 (4): 327-328

    View details for PubMedID 10102673

  • Lymphedema: classification, diagnosis and therapy. Vascular medicine Szuba, A., Rockson, S. G. 1998; 3 (2): 145-156

    Abstract

    This review presents the diagnostic features, the pathophysiology and the available therapies for lymphedema. This disease is often able to be diagnosed by its characteristic clinical presentation, yet, in some cases, ancillary tests might be necessary to establish the diagnosis, particularly in the early stages of the disease and in edemas of mixed etiology. These diagnostic modalities are also useful in clinical studies. Available modalities include isotopic lymphoscintigraphy, indirect and direct lymphography, magnetic resonance imaging, computed tomography and ultrasonography. Lymphedema may be primary or secondary to the presence of other disease and/or to the consequences of surgery. Primary lymphedema may occur at any phase of life but it most commonly appears at puberty. Secondary lymphedema is encountered more often. The most prevalent worldwide cause of lymphedema is filariasis, which is particularly common in south-east Asia. In the USA, postsurgical lymphedema of the extremity prevails. Complications of chronic limb lymphedema include recurrent cellulitis and lymphangiosarcoma. Most patients are treated conservatively, by means of various forms of compression therapy, including complex physical therapy, pneumatic pumps and compressive garments. Volume reducing surgery is performed rarely. Lymphatic microsurgery is still in an experimental stage, although a few centers consistently report favorable outcomes.

    View details for PubMedID 9796078

  • Peripheral arterial insufficiency: mechanisms, natural history, and therapeutic options. Advances in internal medicine Rockson, S. G., Cooke, J. P. 1998; 43: 253-277

    View details for PubMedID 9506185

  • Lymphedema: anatomy, physiology and pathogenesis. Vascular medicine Szuba, A., Rockson, S. G. 1997; 2 (4): 321-326

    Abstract

    The authors review the current understanding of lymphatic anatomy and physiology, and the pathophysiology of lymphedema. The skin lymphatic system consists of the initial lymphatics, which converge into lymphatic precollectors, collectors and lymphatic ducts; these in turn convey the lymph to the regional lymph nodes. Interstitial fluid and particles enter the initial lymphatics through interendothelial openings and by vesicular transport. Lymphatic uptake is enhanced by external compression. Lymphatic transport depends greatly on contraction of lymphangions, which generate the suction force that promotes absorption of interstitial fluid and expels lymph to collecting ducts. In lymphedema, various types of congenital and acquired abnormalities of lymphatic vessels and lymph nodes have been observed. These often lead to lymphatic hypertension, valvular insufficiency and lymphostasis. Accumulation of interstitial and lymphatic fluid within the skin and subcutaneous tissue stimulates fibroblasts, keratinocytes and adipocytes eventuating in the deposition of collagen and glycosaminoglycans within the skin and subcutaneous tissue together with skin hypertrophy and destruction of elastic fibers.

    View details for PubMedID 9575606

  • Limitations of Quantitative Coronary Angiography Guidebook to Coronary Endovascular Diagnostic Techniques. Geschwind HJ, Kern MJ, Editors. Futura Publications, Mt. Kisko, NY, Rockson S. 1997
  • Lymphedema: A review of the relevant anatomy and physiology of the lymphatics. Vascular Medicine Rockson S., Szuba A. 1997: 321-6
  • High prevalence of venous disease in patients with post mastectomy lymphedema Szuba, A., Hu, B. S., Brittain, J., Rockson, S. G., Cooke, J. P. LIPPINCOTT WILLIAMS & WILKINS. 1996: 1370–70
  • A novel therapy for lymphedema complicated by lymphorrhea. Vascular medicine Szuba, A., Cooke, J. P., Rockson, S. G. 1996; 1 (4): 247-250

    Abstract

    Lymphorrhea is a rarely described complication of chronic lymphedema, in which the disrupted flow through diseased lymphatic channels gives rise to the external drainage of lymph, often heralded by the presence of an enlarging lymphocele. This report documents the applicability of the Reid sleeve, a novel, conservative form of therapy, in an unusually severe and protracted example of lymphorrhea.

    View details for PubMedID 9552579

  • Pregnancy-associated group B streptococcal endocarditis: a report of two fatal cases. Obstetrics and gynecology Sexton, D. J., Rockson, S. G., Hempling, R. E., CATHEY, C. W. 1985; 66 (3): 44S-47S

    Abstract

    Group B streptococci commonly colonize parturient women, yet pregnancy-associated endocarditis due to this organism is rare. Most reports of group B streptococcal endocarditis are from the preantibiotic era and occurred in women with rheumatic mitral valve disease. Reported herein are two cases of fatal group B streptococcal endocarditis involving the aortic valve of women with no preexisting heart disease. One had undergone a second-trimester abortion and the other had a normal pregnancy and uncomplicated vaginal delivery.

    View details for PubMedID 3895083

  • PREGNANCY-ASSOCIATED GROUP-B STREPTOCOCCAL ENDOCARDITIS - A REPORT OF 2 FATAL CASES OBSTETRICS AND GYNECOLOGY Sexton, D. J., Rockson, S. G., Hempling, R. E., CATHEY, C. W. 1985; 66 (3): S44-S47

    Abstract

    Group B streptococci commonly colonize parturient women, yet pregnancy-associated endocarditis due to this organism is rare. Most reports of group B streptococcal endocarditis are from the preantibiotic era and occurred in women with rheumatic mitral valve disease. Reported herein are two cases of fatal group B streptococcal endocarditis involving the aortic valve of women with no preexisting heart disease. One had undergone a second-trimester abortion and the other had a normal pregnancy and uncomplicated vaginal delivery.

    View details for Web of Science ID A1985APU2400015

  • PURIFICATION AND CHARACTERIZATION OF THE MAMMALIAN BETA-2-ADRENERGIC RECEPTOR BIOCHEMISTRY Homcy, C. J., Rockson, S. G., COUNTAWAY, J., Egan, D. A. 1983; 22 (3): 660-668

    View details for Web of Science ID A1983QA68000021

    View details for PubMedID 6301525

  • AN ANTIIDIOTYPIC ANTIBODY THAT RECOGNIZES THE BETA-ADRENERGIC-RECEPTOR JOURNAL OF CLINICAL INVESTIGATION Homcy, C. J., Rockson, S. G., Haber, E. 1982; 69 (5): 1147-1154

    Abstract

    Antialprenolol rabbit antibodies were fractionated on an acebutolol affinity resin, followed by L-propranolol elution so as to separate a class of binding sites that mimic the beta-adrenergic receptor. Allotype-identicaL rabbits were immunized with this fraction. After 6 mo, antisera exhibited antiidiotypic activity inhibiting [3H]alprenolol binding to the original antibody and to rabbit antiacebutolol antibodies, which had a spectrum of ligand-binding properties identical to the original idiotype. Those antisera demonstrating the original idiotype. Those antisera demonstrating the most potent antiidiotypic activity also blocked [3H]alprenolol binding to the beta-adrenergic receptor of turkey membrane, canine pulmonary membrane, and rat reticulocyte. An idiotype affinity-purified fraction showed similar activity, inhibiting beta-receptor binding with a calculated dissociation constant (KD) of 53 nM. Isoproterenol-mediated adenylate cyclase activity was also inhibited in a competitive manner. The universality of recognition of these antiidiotypic antisera indicate that the three-dimensional structure of a receptor's binding site can be modeled by a subset of an elicited antibody population.

    View details for Web of Science ID A1982NN58300010

    View details for PubMedID 6279698

    View details for PubMedCentralID PMC370179

  • CELLULAR MECHANISMS OF IMPAIRED ADRENERGIC RESPONSIVENESS IN NEONATAL DOGS JOURNAL OF CLINICAL INVESTIGATION Rockson, S. G., Homcy, C. J., QUINN, P., MANDERS, W. T., Haber, E., Vatner, S. F. 1981; 67 (2): 319-327

    Abstract

    The myocardial responsiveness of conscious, instrumental dogs to exogenously administered isoproterenol and norepinephrine was investigated in neonatal, 6-wk-old, and adult animals. Comparable base-line values for peak left ventricular derivative of pressure with respect to time were observed in all age categories. However, when compared with adult responses, the sympathomimetic amine-induced increases in neonatal left ventricular dP/dt were significantly blunted at each concentration of adrenergic agonist examined, whereas the 6-wk-old puppies displayed an intermediate inotropic response. To investigate the cellular mechanisms of this blunted neonatal response, we correlated physiologic and biochemical measurements of the myocardial responses to catecholamines in each age category. When compared with adult myocardial membrane preparations, neonatal cardiac membranes were characterized in vitro by an increased density of beta-adrenergic binding sites, comparable affinity for adrenergic agonists and antagonists, and an enhanced coupling of adenylate cyclase activation to receptor occupancy. Simultaneous changes in either the serum catecholamine concentration or the membrane content of other intrinsic proteins failed to account for the observed neonatal increase in beta-adrenergic receptor density. These findings are most consistent with a compensatory mechanism of the cardiac cell membrane, whereby an inherent depression in the adrenergic responsiveness of the immature myocardium appears to induce the increase in receptor density and activation of adenylate cyclase.

    View details for Web of Science ID A1981LA65700001

    View details for PubMedID 6257759

    View details for PubMedCentralID PMC370571

  • ANTI-ALPRENOLOL ANTIBODIES IN THE RABBIT - A NEW PROBE FOR THE STUDY OF BETA-ADRENERGIC-RECEPTOR INTERACTION CIRCULATION RESEARCH Rockson, S. G., Homcy, C. J., Haber, E. 1980; 46 (6): 808-813

    Abstract

    We immunized rabbits with an antigen prepared by covalent linkage of alprenolol, a beta-adrenergic receptor antagonist, to bovine serum albumin. Competitive inhibition of [3H]dihydroalprenolol binding to antisera with a variety of unlabeled ligands revealed broad antibody specificity for beta-adrenergic antagonists and agonists. The antiserum was subjected to affintiy fractionation on hydroxybenzylpindolol-Sepharose 4B. Successive elution with 100 mM Tris HCl, 1M NaCl, 4 M LiBr, and 5 M guanidine yielded fractions with increasing affintiy for hydroxybenzylpindolol. The ligand-binding properties of these affinity-fractionated antibodies suggest that certain of these fractions recognize structural aspects of individual beta-adrenergic ligands which are irrelevant to their biological activity, whereas others can be used to distinguish shared functional properties, such as the ethanolamine side chain, within the structural heterogeneity of beta-adrenergic drugs. In particular, elution of hydroxybenzylpindolol-adsorbed antibody with (-)-propranolol allowed identification of an antibody fraction specific for the (-)-stereoisomer. Thus, affinity fractionation of antibodies raised against beta-adrenergic ligands can provide useful analogues for the further study of the recognition properties of the beta-adrenergic receptor.

    View details for Web of Science ID A1980JW90400010

    View details for PubMedID 6247081

  • PLASMA DOPAMINE-BETA-HYDROXYLASE IN DIAGNOSIS OF NEUROBLASTOMA CANCER Rockson, S. G., Stone, R. A., ODERE, F., GUNNELLS, J. C. 1976; 37 (1): 386-389

    Abstract

    An atypical case of neuroblastoma is described, in which the diagnosis was facilitated by the application of a new biochemical procedure, the assay of plasma dopamine-beta-hydroxylase activity. This laboratory tool is proposed as a useful adjunct to established techniques in the diagnosis of neural crest tumors.

    View details for Web of Science ID A1976BF17600047

    View details for PubMedID 1247966

  • PLASMA DOPAMINE-BETA-HYDROXYLASE ACTIVITY IN ORAL-CONTRACEPTIVE HYPERTENSION CIRCULATION Rockson, S. G., Stone, R. A., GUNNELLS, J. C., Schanberg, S. M., KIRSHNER, N., Robinson, R. R. 1975; 51 (5): 916-923

    Abstract

    A prospective study was undertaken to evaluate the relative contribution of changes in sympathetic nervous system activity, as reflected by changes in dopamine-beta-hydroxylase (DBH) activity, to the pathogenesis of oral contraceptive-induced hypertension. Precontraceptive and serial post contraceptive determinations of blood pressure, plasma renin activity (PRA), DBH activity, and changes in body weight were obtained in twelve control patients and forty-one oral contraceptive users. Forty-four percent of oral contraceptive users had increases in blood pressure but remained normotensive and 17% became frankly hypertensive. The precontraceptive and average post contraceptive levels of mean arterial pressure (MAP), PRA and DBH activity in each patient were compared using paired group analysis. Control patients (group I) exhibited no significant changes in these variables, while the patients with contraceptive-induced increases in MAP (groups III and IV) underwent significant, parallel increases in DBH activity. Finally, the linear regression of changes in MAP on the percent change in DBH activity was examined. The positive slopes in groups III and IV differed significantly from the negative slope of the controls (group I). The data have been interpreted to reflect an inappropriate oral contraceptive-induced stimulus to sympathetic nervous system activity, leading to increases in MAP in susceptible individuals.

    View details for Web of Science ID A1975AA03800021

    View details for PubMedID 1122595

  • LESCH-NYHAN SYNDROME - EVIDENCE FOR ABNORMAL ADRENERGIC FUNCTION SCIENCE Rockson, S., Stone, R., VANDERWE, M., Kelley, W. N. 1974; 186 (4167): 934-935

    Abstract

    Subjects with the Lesch-Nyhan syndrome (hypoxanthine-guanine phosphoribosyltransferase deficiency with self-mutilation) exhibit an apparently unique pattern of adrenergic dysfunction characterized by elevated plasma dopamine beta-hydroxylase activity and an absence of pressor response to acute sympathetic stimulation. Patients with a partial deficiency of hypoxanthine-guanine phosphoribosyltransferase without self-mutilation do not exhibit these abnormalities of adrenergic function.

    View details for Web of Science ID A1974U773500024

    View details for PubMedID 4469689

  • SOLITARY RENAL CYST WITH SEGMENTAL ISCHEMIA AND HYPERTENSION JOURNAL OF UROLOGY Rockson, S. G., Stone, R. A., GUNNELLS, J. C. 1974; 112 (5): 550-552

    View details for Web of Science ID A1974U697800004

    View details for PubMedID 4424446