Stanford University

Showing 1-10 of 165 Results

• 

  Raya Saab

  Lindhard Family Professor of Pediatric Cancer Biology
  

  BioI am a pediatric oncologist, and I primarily treat children who are diagnosed with soft tissue sarcomas including rhabdomyosarcoma, and children diagnosed with the eye tumor retinoblastoma, as well as children with other solid tumors.
  I have two very different areas of primary research interest, both of which I pursue with passion. One focuses on global oncology, including clinical and research resource capacity building towards effective treatment and improving outcomes of children with cancer worldwide. I work with collaborators across the globe towards a common goal of improving access to diagnostic and clinical care, training of multidisciplinary teams, and building clinical resources and research capacity to develop context-informed approaches to improving cancer care and achieving better outcomes for children diagnosed with cancer irrespective of where they happen to live.
  My parallel research interest, which is the focus of my laboratory, is understanding oncogenic signaling in pediatric soft tissue sarcomas, in an effort to clarify the driving biology and determinants of metastatic disease, to uncover novel targets for more effective treatment. We use preclinical in vitro and in vivo models, including murine and human cell lines, and mouse models of cancer. We have recently uncovered a paracrine role for rhabdomyosarcoma-secreted exosomes in impacting biology of stromal cells. Rhabdomyosarcoma-derived exosomes carry specific miRNA cargo that imparts an invasive and migratory phenotype on normal recipient fibroblasts, and proteomic analysis revealed specific and unique pathways relevant to the two different molecular rhabdomyosarcoma subtypes that are driven by distinct oncogenic pathways. We identified that the driver oncogene in fusion-positive rhabdomyosarcoma, PAX3-FOXO1, modulates exosome cargo to promote invasion, migration, and angiogenic properties, and identified specific microRNA and protein cargo acting as effectors of PAX3-FOXO1 exosome-mediated signaling, including modulation of oxidative stress response and cell survival signaling. Our ongoing work is focused on interrogating specific paracrine signaling pathways and molecular mechanisms of metastatic disease progression in rhabdomyosarcoma, for potential therapeutic targeting.

  • Contact Info

    Mail Code: 5798

    rsaab@stanford.edu
• 

  Pauline Sadrieh

  Affiliate, Pediatrics - Pulmonary Medicine
  
• 

  Rebecca Saenz

  Clinical Assistant Professor, Pediatrics - Immunology
  

  Current Research and Scholarly InterestsAllergy, Immunology, Bioengineering and Biodesign

  • Contact Info

    Mail Code: 5366

    rksaenz@stanford.edu

  • Other Names:

    Becca Saenz
• 

  Cristina Maria Saez

  Clinical Assistant Professor, Pediatrics - Rheumatology
  

  • Contact Info

    Mail Code: 5731

    csaez@stanford.edu
• 

  Julien Sage

  Elaine and John Chambers Professor of Pediatric Cancer and Professor of Genetics
  

  Current Research and Scholarly InterestsWe investigate the mechanisms by which normal cells become tumor cells, and we combine genetics, genomics, and proteomics approaches to investigate the differences between the proliferative response in response to injury and the hyperproliferative phenotype of cancer cells and to identify novel therapeutic targets in cancer cells.

  • Contact Info

    • Stanford University, School of Medicine
    • Department of Pediatrics
    • 265 Campus Drive, SIM1 Lokey Building, Room 2078a
    • Stanford, California 94305-5457

    Mail Code: 5457

    julsage@stanford.edu

  • Web page:

    http://web.stanford.edu/group/sage
• Julieanna Sahouria-Rukab

  Clinical Instructor (Affiliated), Pediatrics - General Pediatrics
  
• 

  Neetu Saini

  Postdoctoral Scholar, Stem Cell Transplantation
  

  BioMy research interests focus on translational human T-cell immunology, with an emphasis on regulatory T cells (Tregs) and their therapeutic potential in restoring immune tolerance and tissue homeostasis. I am particularly interested in engineering FOXP3-programmed CD4⁺ T cells as a stable and functional alternative to conventional Tregs, especially in inflammatory settings where endogenous Tregs may be unstable or dysfunctional. My work integrates gene-editing approaches, immunophenotyping, and human organoid systems to study how these engineered cells interact with epithelial and stem cell compartments, with a focus on mechanisms of tissue repair and immune–epithelial crosstalk in barrier tissues such as the intestine. Moving forward, I aim to advance next-generation cell therapies by combining insights from T-cell biology, tissue biology, and disease modeling to develop durable and clinically relevant strategies for treating immune-mediated and epithelial barrier disorders.

  • Contact Info

    Mail Code: 5660

    neetus@stanford.edu
• Tanya Saini

  Research Assistant, Pediatrics - Rheumatology
  

  • Contact Info

    Mail Code: 5208

    tsaini@stanford.edu
• Adele Saives

  Graduate, Medicine, Pediatrics
  

  • Contact Info

    asaives@stanford.edu
• 

  Debbie C. Sakaguchi Sakai

  Clinical Professor, Pediatrics
  

  Current Research and Scholarly InterestsMedical education, shared decision making, resuscitation.

  • Contact Info

    • 453 Quarry Rd
    • Center For Academic Medicine
    • Palo Alto, California 94304-1419

    Mail Code: 5776

    • (650) 736-4423 (office)

    (650) 736-6690 (fax)