作者
Ning Ma,Yi-Kang Wang,Sheng Xu,Qian-Zhi Ni,Qian-Wen Zheng,Bing Zhu,Hui-Jun Cao,Hao Jiang,Fei Zhang,Yan-Mei Yuan,Er-Bin Zhang,Tian-Wei Chen,Ji Xia,Xu-Fen Ding,Zhen-Hua Chen,Xiu-Ping Zhang,Kang Wang,Shu-Qun Cheng,Lin Qiu,Zhigang Li,Yong-Chun Yu,Xiao-Fan Wang,Bin Zhou,Jingjing Li,Dong Xie
摘要
Abstract Non-alcoholic fatty liver disease (NAFLD) has become the most prevalent chronic liver disease in the world, however, no drug treatment has been approved for this disease. Thus, it is urgent to find effective therapeutic targets for clinical intervention. In this study, we find that liver-specific knockout of PPDPF (PPDPF-LKO) leads to spontaneous fatty liver formation in a mouse model at 32 weeks of age on chow diets, which is enhanced by HFD. Mechanistic study reveals that PPDPF negatively regulates mTORC1-S6K-SREBP1 signaling. PPDPF interferes with the interaction between Raptor and CUL4B-DDB1, an E3 ligase complex, which prevents ubiquitination and activation of Raptor. Accordingly, liver-specific PPDPF overexpression effectively inhibits HFD-induced mTOR signaling activation and hepatic steatosis in mice. These results suggest that PPDPF is a regulator of mTORC1 signaling in lipid metabolism, and may be a potential therapeutic candidate for NAFLD.