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SMRT-GPS2 corepressor pathway dysregulation coincides with obesity-linked adipocyte inflammation
Amine Toubal, … , Eckardt Treuter, Nicolas Venteclef
Amine Toubal, … , Eckardt Treuter, Nicolas Venteclef
Published December 10, 2012
Citation Information: J Clin Invest. 2013;123(1):362-379. https://doi.org/10.1172/JCI64052.
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Research Article Inflammation

SMRT-GPS2 corepressor pathway dysregulation coincides with obesity-linked adipocyte inflammation

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Abstract

Low-grade chronic inflammation is a major characteristic of obesity and results from deregulated white adipose tissue function. Consequently, there is interest in identifying the underlying regulatory mechanisms and components that drive adipocyte inflammation. Here, we report that expression of the transcriptional corepressor complex subunits GPS2 and SMRT was significantly reduced in obese adipose tissue, inversely correlated to inflammatory status, and was restored upon gastric bypass surgery–induced weight loss in morbid obesity. These alterations correlated with reduced occupancy of the corepressor complex at inflammatory promoters, providing a mechanistic explanation for elevated inflammatory transcription. In support of these correlations, RNAi-mediated depletion of GPS2 and SMRT from cultured human adipocytes promoted derepression of inflammatory transcription and elevation of obesity-associated inflammatory markers, such as IL-6 and MCP-1. Furthermore, we identified a regulatory cascade containing PPARγ and TWIST1 that controlled the expression of GPS2 and SMRT in human adipocytes. These findings were clinically relevant, because treatment of diabetic obese patients with pioglitazone, an antidiabetic and antiinflammatory PPARγ agonist, restored expression of TWIST1, GPS2, and SMRT in adipose tissue. Collectively, our findings identify alterations in a regulatory transcriptional network in adipocytes involving the dysregulation of a specific corepressor complex as among the initiating events promoting adipose tissue inflammation in human obesity.

Authors

Amine Toubal, Karine Clément, Rongrong Fan, Patricia Ancel, Veronique Pelloux, Christine Rouault, Nicolas Veyrie, Agnes Hartemann, Eckardt Treuter, Nicolas Venteclef

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Figure 2

Adipocyte inflammation is associated with clearance of the SMRT-GPS2 complex from the IL-6 promoter.

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Adipocyte inflammation is associated with clearance of the SMRT-GPS2 com...
(A–E) qPCR analysis of mRNA expression of SMRT, GPS2, NCOR1, adiponectin, and IL-6 in isolated human adipocytes from subcutaneous adipose tissue of lean (n = 8) and obese (n = 12) subjects. *P < 0.05. (F–H) Gene expression correlations were analyzed using Spearman statistical test. (I) Western blot analysis of protein levels of GPS2, SMRT, and NCOR1 in isolated human mature adipocytes from subcutaneous adipose tissue of lean and obese subjects (n = 3). (J) ChIP assays were performed to measure recruitment of GPS2, SMRT, NCOR1, HDAC3, and POL2 onto the IL-6 promoter, in conjunction with histone modifications (me2H3K9, indicative of repression, and me2H3K4 and acH3, indicative of activation), in isolated human adipocytes from subcutaneous adipose tissue of lean (n = 6) and obese (n = 5) subjects. IgG served as nonspecific control antibody.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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