Clonal analyses and gene profiling identify genetic biomarkers of the thermogenic potential of human brown and white preadipocytes

脂肪生成 生物 产热 白色脂肪组织 产热素 褐色脂肪组织 脂肪组织 内分泌学 细胞生物学
作者
Ruidan Xue,Matthew D. Lynes,Jonathan M. Dreyfuss,Farnaz Shamsi,Tim J. Schulz,Hongbin Zhang,Tian Lian Huang,Kristy L. Townsend,Yiming Li,Hirokazu Takahashi,Lauren S Weiner,Andrew P. White,Maureen S. Lynes,Lee L. Rubin,Laurie J. Goodyear,Aaron M. Cypess,Yu‐Hua Tseng
出处
期刊:Nature Medicine [Nature Portfolio]
卷期号:21 (7): 760-768 被引量:306
标识
DOI:10.1038/nm.3881
摘要

Human brown and white preadipocyte clones from neck fat depots have been isolated and used to identify genetic biomarkers that predict their thermogenic capacity. Targeting brown adipose tissue (BAT) content or activity has therapeutic potential for treating obesity and the metabolic syndrome by increasing energy expenditure. However, both inter- and intra-individual differences contribute to heterogeneity in human BAT and potentially to differential thermogenic capacity in human populations. Here we generated clones of brown and white preadipocytes from human neck fat and characterized their adipogenic and thermogenic differentiation. We combined an uncoupling protein 1 (UCP1) reporter system and expression profiling to define novel sets of gene signatures in human preadipocytes that could predict the thermogenic potential of the cells once they were maturated. Knocking out the positive UCP1 regulators, PREX1 and EDNRB, in brown preadipocytes using CRISPR-Cas9 markedly abolished the high level of UCP1 in brown adipocytes differentiated from the preadipocytes. Finally, we were able to prospectively isolate adipose progenitors with great thermogenic potential using the cell surface marker CD29. These data provide new insights into the cellular heterogeneity in human fat and offer potential biomarkers for identifying thermogenically competent preadipocytes.
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