作者
Yingxu Ma, Shanshan Liu, Heejin Jun, Jine Wang, Xiaoli Fan, Guobing Li, Lei Yin, Liangyou Rui, Steven A Weinman, Jianke Gong, Jun Wu
发表日期
2020/11
期刊
FASEB journal: official publication of the Federation of American Societies for Experimental Biology
卷号
34
期号
11
页码范围
14863
出版商
NIH Public Access
简介
Appropriate control of hepatic gluconeogenesis is essential for the organismal survival upon prolonged fasting and maintaining systemic homeostasis under metabolic stress. Here we show protein arginine methyltransferase 1 (PRMT1), a key enzyme that catalyzes the protein arginine methylation process, particularly the isoform encoded by Prmt1 variant 2 (PRMT1V2), is critical in regulating gluconeogenesis in the liver. Liver-specific deletion of Prmt1 reduced gluconeogenic capacity in cultured hepatocytes and in the liver. Prmt1v2 was expressed at a higher level compared to Prmt1v1 in hepatic tissue and cells. Gain-of-function of PRMT1V2 clearly activated the gluconeogenic program in hepatocytes via interactions with PGC1α, a key transcriptional coactivator regulating gluconeogenesis, enhancing its activity via arginine methylation, while no effects of PRMT1V1 were observed. Similar stimulatory effects of …
引用总数
20212022202320241313
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