| Literature DB >> 30943403 |
Matthew J Harms1, Qian Li2, Sunjae Lee3, Cheng Zhang3, Bengt Kull1, Stefan Hallen1, Anders Thorell4, Ida Alexandersson1, Carolina E Hagberg5, Xiao-Rong Peng1, Adil Mardinoglu6, Kirsty L Spalding7, Jeremie Boucher8.
Abstract
White adipose tissue (WAT) is a central factor in the development of type 2 diabetes, but there is a paucity of translational models to study mature adipocytes. We describe a method for the culture of mature white adipocytes under a permeable membrane. Compared to existing culture methods, MAAC (membrane mature adipocyte aggregate cultures) better maintain adipogenic gene expression, do not dedifferentiate, display reduced hypoxia, and remain functional after long-term culture. Subcutaneous and visceral adipocytes cultured as MAAC retain depot-specific gene expression, and adipocytes from both lean and obese patients can be cultured. Importantly, we show that rosiglitazone treatment or PGC1α overexpression in mature white adipocytes induces a brown fat transcriptional program, providing direct evidence that human adipocytes can transdifferentiate into brown-like adipocytes. Together, these data show that MAAC are a versatile tool for studying phenotypic changes of mature adipocytes and provide an improved translational model for drug development.Entities:
Keywords: BAT; MAAC; UCP1; WAT; adipocyte; brown adipose; culture; transdifferentiation; white adipose
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Year: 2019 PMID: 30943403 DOI: 10.1016/j.celrep.2019.03.026
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423