Fas (CD95) in adipocytes mediates adipose tissue inflammation and contributes to liver and whole-body insulin resistance

Autor: Wueest Stephan, Rapold Reto A, Schumann Desiree M, Rytka Julia M, Schildknecht Anita, Nov Ori, Chervonsky Alexander V, Rudich Assaf, Schoenle Eugen J, Donath Marc Y, Konrad Daniel
Rok vydání: 2010
Zdroj: The Journal of clinical investigation
DOI: 10.1172/JCI38388
Popis: Adipose tissue inflammation is linked to the pathogenesis of insulin resistance. In addition to exerting death promoting effects the death receptor Fas (also known as CD95) can activate inflammatory pathways in several cell lines and tissues although little is known about the metabolic consequence of Fas activation in adipose tissue. We therefore sought to investigate the contribution of Fas in adipocytes to obesity associated metabolic dysregulation. Fas expression was markedly increased in the adipocytes of common genetic and diet induced mouse models of obesity and insulin resistance as well as in the adipose tissue of obese and type 2 diabetic patients. Mice with Fas deficiency either in all cells or specifically in adipocytes (the latter are referred to herein as AFasKO mice) were protected from deterioration of glucose homeostasis induced by high fat diet (HFD). Adipocytes in AFasKO mice were more insulin sensitive than those in wild type mice and mRNA levels of proinflammatory factors were reduced in white adipose tissue. Moreover AFasKO mice were protected against hepatic steatosis and were more insulin sensitive both at the whole body level and in the liver. Thus Fas in adipocytes contributes to adipose tissue inflammation hepatic steatosis and insulin resistance induced by obesity and may constitute a potential therapeutic target for the treatment of insulin resistance and type 2 diabetes.
Databáze: OpenAIRE