| Literature DB >> 31974143 |
Jian-Hui Shi1, Jun-Yu Lu1, Heng-Yu Chen2, Chun-Chun Wei3, Xiongfei Xu1, Hao Li3, Qiufang Bai1,4, Fang-Zhen Xia5, Sin Man Lam6, Hai Zhang3, Ya-Nan Shi4, Dongmei Cao1, Liming Chen2, Guanghou Shui6, Xia Yang7, Yingli Lu8, Yu-Xia Chen3, Weiping J Zhang3,4.
Abstract
Excessive fructose consumption is closely linked to the pathogenesis of metabolic disease. Carbohydrate response element-binding protein (ChREBP) is a transcription factor essential for fructose tolerance in mice. However, the functional significance of liver ChREBP in fructose metabolism remains unclear. Here, we show that liver ChREBP protects mice against fructose-induced hepatotoxicity by regulating liver glycogen metabolism and ATP homeostasis. Liver-specific ablation of ChREBP did not compromise fructose tolerance, but rather caused severe transaminitis and hepatomegaly with massive glycogen overload in mice fed a high-fructose diet, while no obvious inflammation, cell death, or fibrosis was detected in the liver. In addition, liver ATP contents were significantly decreased by ChREBP deficiency in the fed state, which was rendered more pronounced by fructose feeding. Mechanistically, liver contents of glucose-6-phosphate (G6P), an allosteric activator of glycogen synthase, were markedly increased in the absence of liver ChREBP, while fasting-induced glycogen breakdown was not compromised. Furthermore, hepatic overexpression of LPK, a ChREBP target gene in glycolysis, could effectively rescue glycogen overload and ATP reduction, as well as mitigate fructose-induced hepatotoxicity in ChREBP-deficient mice. Taken together, our findings establish a critical role of liver ChREBP in coping with hepatic fructose stress and protecting from hepatotoxicity by regulating LPK.Entities:
Year: 2020 PMID: 31974143 DOI: 10.2337/db19-0388
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461