Eric Sager Luxenberg
Ph.D. Student in Electrical Engineering, admitted Autumn 2020
All Publications
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Portfolio Optimization with Cumulative Prospect Theory Utility via Convex Optimization
COMPUTATIONAL ECONOMICS
2024
View details for DOI 10.1007/s10614-024-10556-x
View details for Web of Science ID 001159490000001
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Portfolio construction with Gaussian mixture returns and exponential utility via convex optimization
OPTIMIZATION AND ENGINEERING
2023
View details for DOI 10.1007/s11081-023-09814-y
View details for Web of Science ID 001037322900001
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Strategic Asset Allocation with Illiquid Alternatives
ASSOC COMPUTING MACHINERY. 2022: 249-256
View details for DOI 10.1145/3533271.3561769
View details for Web of Science ID 001103234000030
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Discovery of surrogate agonists for visceral fat Treg cells that modulate metabolic indices in vivo.
eLife
2020; 9
Abstract
T regulatory (Treg) cells play vital roles in modulating immunity and tissue homeostasis. Their actions depend on TCR recognition of peptide-MHC molecules; yet the degree of peptide specificity of Treg-cell function, and whether Treg ligands can be used to manipulate Treg cell biology are unknown. Here, we developed an Ab-peptide library that enabled unbiased screening of peptides recognized by a bona fide murine Treg cell clone isolated from the visceral adipose tissue (VAT), and identified surrogate agonist peptides, with differing affinities and signaling potencies. The VAT-Treg cells expanded in vivo by one of the surrogate agonists preserved the typical VAT-Treg transcriptional programs. Immunization with this surrogate, especially when coupled with blockade of TNFa signaling, expanded VAT-Treg cells, resulting in protection from inflammation and improved metabolic indices, including promotion of insulin sensitivity. These studies suggest that antigen-specific targeting of VAT-localized Treg cells could eventually be a strategy for improving metabolic disease.
View details for DOI 10.7554/eLife.58463
View details for PubMedID 32773038
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Using machine learning to discover shape descriptors for predicting emulsion stability in a microfluidic channel.
Soft matter
2018
Abstract
In soft matter consisting of many deformable objects, object shapes often carry important information about local forces and their interactions with the local environment, and can be tightly coupled to the bulk properties and functions. In a concentrated emulsion, for example, the shapes of individual droplets are directly related to the local stress arising from interactions with neighboring drops, which in turn determine their stability and the resulting rheological properties. Shape descriptors used in prior work on single drops and dilute emulsions, where droplet-droplet interactions are largely negligible and the drop shapes are simple, are insufficient to fully capture the broad range of droplet shapes in a concentrated system. This paper describes the application of a machine learning method, specifically a convolutional autoencoder model, that learns to: (1) discover a low-dimensional code (8-dimensional) to describe droplet shapes within a concentrated emulsion, and (2) predict whether the drop will become unstable and undergo break-up. The input consists of images (N = 500002) of two-dimensional droplet boundaries extracted from movies of a concentrated emulsion flowing through a confined microfluidic channel as a monolayer. The model is able to faithfully reconstruct droplet shapes, as well as to achieve a classification accuracy of 91.7% in the prediction of droplet break-up, compared with 60% using conventional scalar descriptors based on droplet elongation. It is observed that 4 out of the 8 dimensions of the code are interpretable, corresponding to drop skewness, elongation, throat size, and surface curvature, respectively. Furthermore, the results show that drop elongation, throat size, and surface curvature are dominant factors in predicting droplet break-up for the flow conditions tested. The method presented is expected to facilitate follow-on work to identify the relationship between drop shapes and the interactions with other drops, and to identify potentially new modes of break-up mechanisms in a concentrated system. Finally, the method developed here should also apply to other soft materials such as foams, gels, and cells and tissues.
View details for PubMedID 30570628