Novel Mechanism of Foxo1 Phosphorylation in Glucagon Signaling in Control of Glucose Homeostasis

被引:73
作者
Wu, Yuxin [1 ]
Pan, Quan [1 ]
Yan, Hui [1 ]
Zhang, Kebin [1 ]
Guo, Xiaoqin [2 ,3 ]
Xu, Zihui [1 ]
Yang, Wanbao [1 ]
Qi, Yajuan [1 ]
Guo, Cathy A. [1 ]
Hornsby, Caitlyn [1 ]
Zhang, Lin [4 ]
Zhou, Aimin [4 ]
Li, Ling [1 ]
Chen, Yunmei [1 ]
Zhang, Weiping [1 ]
Sun, Yuxiang [1 ]
Zheng, Hongting [2 ]
Wondisford, Fred [3 ]
He, Ling [3 ]
Guo, Shaodong [1 ]
机构
[1] Texas A&M Univ, Coll Agr & Life Sci, Dept Nutr & Food Sci, College Stn, TX USA
[2] Third Mil Med Univ, Dept Endocrinol, Chongqing, Peoples R China
[3] Johns Hopkins Univ, Dept Med, Div Endocrinol, Baltimore, MD USA
[4] Cleveland State Univ, Dept Chem, Cleveland, OH 44115 USA
基金
美国国家卫生研究院; 美国食品与农业研究所;
关键词
GROWTH-FACTOR; PEPTIDE-1; RECEPTOR; DEFICIENT MICE; IN-VIVO; LIVER; SATIETY; MTOR; RESPONSIVENESS; CONTRIBUTE; RESISTANCE;
D O I
10.2337/db18-0674
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Dysregulation of hepatic glucose production (HGP) serves as a major underlying mechanism for the pathogenesis of type 2 diabetes. The pancreatic hormone glucagon increases and insulin suppresses HGP, controlling blood glucose homeostasis. The forkhead transcription factor Foxo1 promotes HGP through increasing expression of genes encoding the rate-limiting enzymes responsible for gluconeogenesis. We previously established that insulin suppresses Foxo1 by Akt-mediated phosphorylation of Foxo1 at Ser(256) in human hepatocytes. In this study, we found a novel Foxo1 regulatory mechanism by glucagon, which promotes Foxo1 nuclear translocation and stability via cAMP- and protein kinase A-dependent phosphorylation of Foxo1 at Ser(276). Replacing Foxo1-S276 with alanine (A) or aspartate (D) to block or mimic phosphorylation, respectively, markedly regulates Foxo1 stability and nuclear localization in human hepatocytes. To establish in vivo function of Foxo1-Ser(276) phosphorylation in glucose metabolism, we generated Foxo1-S273A and Foxo1-S273D knock-in (KI) mice. The KI mice displayed impaired blood glucose homeostasis, as well as the basal and glucagon-mediated HGP in hepatocytes. Thus, Foxo1-Ser(276) is a new target site identified in the control of Foxo1 bioactivity and associated metabolic diseases.
引用
收藏
页码:2167 / 2182
页数:16
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