CDK6 inhibits de novo lipogenesis in white adipose tissues but not in the liver

Author:

Hu Alexander J.,Li Wei,Dinh Calvin,Zhang Yongzhao,Hu Jamie K.,Daniele Stefano G.,Hou Xiaoli,Yang ZixuanORCID,Asara John M.,Hu Guo-fuORCID,Farmer Stephen R.ORCID,Hu Miaofen G.ORCID

Abstract

AbstractIncreased de novo lipogenesis (DNL) in white adipose tissue is associated with insulin sensitivity. Under both Normal-Chow-Diet and High-Fat-Diet, mice expressing a kinase inactive Cyclin-dependent kinase 6 (Cdk6) allele (K43M) display an increase in DNL in visceral white adipose tissues (VAT) as compared to wild type mice (WT), accompanied by markedly increased lipogenic transcriptional factor Carbohydrate-responsive element-binding proteins (CHREBP) and lipogenic enzymes in VAT but not in the liver. Treatment of WT mice under HFD with a CDK6 inhibitor recapitulates the phenotypes observed in K43M mice. Mechanistically, CDK6 phosphorylates AMP-activated protein kinase, leading to phosphorylation and inactivation of acetyl-CoA carboxylase, a key enzyme in DNL. CDK6 also phosphorylates CHREBP thus preventing its entry into the nucleus. Ablation of runt related transcription factor 1 in K43M mature adipocytes reverses most of the phenotypes observed in K43M mice. These results demonstrate a role of CDK6 in DNL and a strategy to alleviate metabolic syndromes.

Publisher

Springer Science and Business Media LLC

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