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Probing Insulin Sensitivity with Metabolically Competent Human Stem Cell-Derived White Adipose Tissue Microphysiological Systems

Small. 2021-11; 
Lin Qi, Peter-James H Zushin, Ching-Fang Chang, Yue Tung Lee, Diana L Alba, Suneil K Koliwad, Andreas Stahl
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Proteins, Expression, Isolation and Analysis … Prior to cell loading, 10 wt% MMP cleavable peptides (CQPQGLAKC, GenScript) were dissolved in TEOA and directly added to the cell pellet with dissolved HA precursor under a peptide-to-precursor volume ratio of 1:10. The hydrogel-cell mixture was injected into the cell … Get A Quote

摘要

Impaired white adipose tissue (WAT) function has been recognized as a critical early event in obesity-driven disorders, but high buoyancy, fragility, and heterogeneity of primary adipocytes have largely prevented their use in drug discovery efforts highlighting the need for human stem cell-based approaches. Here, human stem cells are utilized to derive metabolically functional 3D adipose tissue (iADIPO) in a microphysiological system (MPS). Surprisingly, previously reported WAT differentiation approaches create insulin resistant WAT ill-suited for type-2 diabetes mellitus drug discovery. Using three independent insulin sensitivity assays, i.e., glucose and fatty acid uptake and suppression of lipolysis, as the ... More

關(guān)鍵詞

human-induced pluripotent stem cells, insulin sensitivity, microphysiological system, organ-on-a-chip, white adipose tissue
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