Reduced subcutaneous adipogenesis in human hypertrophic obesity is linked to senescent precursor cells
- PMID: 31227697
- PMCID: PMC6588633
- DOI: 10.1038/s41467-019-10688-x
Reduced subcutaneous adipogenesis in human hypertrophic obesity is linked to senescent precursor cells
Abstract
Inappropriate expansion of the adipose cells in the subcutaneous adipose tissue (SAT) is a characteristic of hypertrophic obesity and of individuals with genetic predisposition for T2D (first-degree relatives; FDR). It is associated with insulin resistance, a dysfunctional, adipose tissue and reduced adipogenesis. We examined the regulation of adipogenesis in human SAT precursor cells and found ZNF521 to be a critical regulator of early adipogenic commitment and precursor cells leaving the cell cycle. However, neither altered upstream signalling nor lack of SAT progenitor cells could explain the reduced adipogenesis in hypertrophic obesity. Instead, we show that progenitor cells undergoing poor differentiation are characterized by senescence, inability to suppress p53/P16INK4 and secretion of factors reducing adipogenesis in non-senescent cells. We found aging, FDR and established T2D to be associated with increased progenitor cell senescence, reduced adipogenesis and hypertrophic expansion of the SAT adipose cells.
Conflict of interest statement
The authors declare no competing interests.
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- K2013-54X-03506-42-5/Vetenskapsrådet (Swedish Research Council)/International
- DIA2016-108/Diabetesförbundet (Svenska Diabetesförbundet)/International
- NNF17OC0026712/Novo Nordisk Foundation Center for Basic Metabolic Research (NovoNordisk Foundation Center for Basic Metabolic Research)/International
- ALFGBG-718601/Sveriges Kommuner och Landsting (Swedish Association of Local Authorities and Regions)/International
- EFSD/NN 2015/European Foundation for the Study of Diabetes (EFSD)/International
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