| Literature DB >> 36217034 |
Chen-Song Zhang1, Mengqi Li1, Yu Wang1, Xiaoyang Li1, Yue Zong1, Shating Long1, Mingliang Zhang2, Jin-Wei Feng1, Xiaoyan Wei1, Yan-Hui Liu1, Baoding Zhang1, Jianfeng Wu3, Cixiong Zhang1, Wenhua Lian1, Teng Ma1, Xiao Tian1, Qi Qu1, Yaxin Yu1, Jinye Xiong1, Dong-Tai Liu1, Zhenhua Wu1, Mingxia Zhu1, Changchuan Xie1, Yaying Wu1, Zheni Xu1, Chunyan Yang1, Junjie Chen4, Guohong Huang1, Qingxia He5, Xi Huang1, Lei Zhang1, Xiufeng Sun1, Qingfeng Liu1, Abdul Ghafoor1, Fu Gui1, Kaili Zheng6, Wen Wang7, Zhi-Chao Wang7, Yong Yu1, Qingliang Zhao6, Shu-Yong Lin1, Zhi-Xin Wang5, Hai-Long Piao7, Xianming Deng8, Sheng-Cai Lin9.
Abstract
The activity of 5'-adenosine monophosphate-activated protein kinase (AMPK) is inversely correlated with the cellular availability of glucose. When glucose levels are low, the glycolytic enzyme aldolase is not bound to fructose-1,6-bisphosphate (FBP) and, instead, signals to activate lysosomal AMPK. Here, we show that blocking FBP binding to aldolase with the small molecule aldometanib selectively activates the lysosomal pool of AMPK and has beneficial metabolic effects in rodents. We identify aldometanib in a screen for aldolase inhibitors and show that it prevents FBP from binding to v-ATPase-associated aldolase and activates lysosomal AMPK, thereby mimicking a cellular state of glucose starvation. In male mice, aldometanib elicits an insulin-independent glucose-lowering effect, without causing hypoglycaemia. Aldometanib also alleviates fatty liver and nonalcoholic steatohepatitis in obese male rodents. Moreover, aldometanib extends lifespan and healthspan in both Caenorhabditis elegans and mice. Taken together, aldometanib mimics and adopts the lysosomal AMPK activation pathway associated with glucose starvation to exert physiological roles, and might have potential as a therapeutic for metabolic disorders in humans.Entities:
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Year: 2022 PMID: 36217034 PMCID: PMC9584815 DOI: 10.1038/s42255-022-00640-7
Source DB: PubMed Journal: Nat Metab ISSN: 2522-5812