| Literature DB >> 27282405 |
Shuai Chen1, Yujia Kang1, Yan Sun1, Yanhong Zhong1, Yanli Li1, Lijuan Deng1, Jin Tao1, Yang Li1, Yingpu Tian1, Yinan Zhao1, Jianghong Cheng1, Wenjie Liu1, Gen-Sheng Feng2, Zhongxian Lu3.
Abstract
Fatty liver disease is a serious health problem worldwide and is the most common cause for chronic liver disease and metabolic disorders. The major challenge in the prevention and intervention of this disease is the incomplete understanding of the underlying mechanism and thus lack of potent therapeutic targets due to multifaceted and interdependent disease factors. In this study, we investigated the role of a signaling adaptor protein, GRB2-associated-binding protein 2 (Gab2), in fatty liver using an animal disease model. Gab2 expression in hepatocytes responded to various disease factor stimulations, and Gab2 knockout mice exhibited resistance to fat-induced obesity, fat- or alcohol-stimulated hepatic steatosis, as well as methionine and choline deficiency-induced steatohepatitis. Concordantly, the forced expression or knockdown of Gab2 enhanced or diminished oleic acid (OA)- or ethanol-induced lipid production in hepatocytes in vitro, respectively. During lipid accumulation in hepatocytes, both fat and alcohol induced the recruitment of PI3K or Socs3 by Gab2 and the activation of their downstream signaling proteins AKT, ERK, and Stat3. Therefore, Gab2 may be a disease-associated protein that is induced by pathogenic factors to amplify and coordinate multifactor-induced signals to govern disease development in the liver. Our research provides a novel potential target for the prevention and intervention of fatty liver disease.Entities:
Keywords: alcoholic fatty liver disease; disease-associated protein; knockout mouse; non-alcoholic fatty liver disease; therapeutic target
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Year: 2016 PMID: 27282405 DOI: 10.1093/jmcb/mjw028
Source DB: PubMed Journal: J Mol Cell Biol ISSN: 1759-4685 Impact factor: 6.216