| Literature DB >> 29874595 |
Yiming Cheng1, Li Jiang1, Susanne Keipert2, Shuyue Zhang1, Andreas Hauser3, Elisabeth Graf4, Tim Strom4, Matthias Tschöp5, Martin Jastroch6, Fabiana Perocchi7.
Abstract
Activation and recruitment of thermogenic cells in human white adipose tissues ("browning") can counteract obesity and associated metabolic disorders. However, quantifying the effects of therapeutic interventions on browning remains enigmatic. Here, we devise a computational tool, named ProFAT (profiling of fat tissue types), for quantifying the thermogenic potential of heterogeneous fat biopsies based on prediction of white and brown adipocyte content from raw gene expression datasets. ProFAT systematically integrates 103 mouse-fat-derived transcriptomes to identify unbiased and robust gene signatures of brown and white adipocytes. We validate ProFAT on 80 mouse and 97 human transcriptional profiles from 14 independent studies and correctly predict browning capacity upon various physiological and pharmacological stimuli. Our study represents the most exhaustive comparative analysis of public data on adipose biology toward quantification of browning after personalized medical intervention. ProFAT is freely available and should become increasingly powerful with the growing wealth of transcriptomics data.Entities:
Keywords: adipocyte; adipose tissue; beige fat; brown fat; gene expression; metabolic syndrome; obesity; thermogenesis; transcriptome; white fat
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Year: 2018 PMID: 29874595 DOI: 10.1016/j.celrep.2018.05.021
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423