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Merck

High-throughput drug screening models of mature adipose tissues which replicate the physiology of patients' Body Mass Index (BMI).

Bioactive materials (2021-09-02)
Fiona Louis, Yoshihiro Sowa, Shiro Kitano, Michiya Matsusaki
ABSTRAKT

Obesity is a complex and incompletely understood disease, but current drug screening strategies mostly rely on immature in vitro adipose models which cannot recapitulate it properly. To address this issue, we developed a statistically validated high-throughput screening model by seeding human mature adipocytes from patients, encapsulated in physiological collagen microfibers. These drop tissues ensured the maintenance of adipocyte viability and functionality for controlling glucose and fatty acids uptake, as well as glycerol release. As such, patients' BMI and insulin sensitivity displayed a strong inverse correlation: the healthy adipocytes were associated with the highest insulin-induced glucose uptake, while insulin resistance was confirmed in the underweight and severely obese adipocytes. Insulin sensitivity recovery was possible with two type 2 diabetes treatments, rosiglitazone and melatonin. Finally, the addition of blood vasculature to the model seemed to more accurately recapitulate the in vivo physiology, with particular respect to leptin secretion metabolism.

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Sigma-Aldrich
Cytochalasin B from Drechslera dematioidea, Ready Made Solution, 10 mg/mL in DMSO
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Rosiglitazone, ≥98% (HPLC)
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Collagenase from Clostridium histolyticum, for general use, Type I, ≥125 CDU/mg solid
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Fibrinogen from bovine plasma, Type I-S, 65-85% protein (≥75% of protein is clottable)
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Thrombin from bovine plasma, lyophilized powder, 40-500 NIH units/mg protein (biuret)
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Bovine Serum Albumin, heat shock fraction, protease free, pH 7, ≥98%
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Glycerol Assay Kit, sufficient for 200 colorimetric or fluorometric tests
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Oleic acid, suitable for cell culture, BioReagent
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Forskolin, For use in molecular biology applications
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Triton X-100, Molecular Biology