| Literature DB >> 30374165 |
Zhimin Huang1, Junxing Zhao1, Wei Deng2, Yingyi Chen1, Jialin Shang1, Kun Song1, Lu Zhang1, Chengxiang Wang1, Shaoyong Lu1, Xiuyan Yang1, Bin He3, Jinrong Min4, Hao Hu5, Minjia Tan5, Jianrong Xu1, Qiufen Zhang1, Jie Zhong1, Xiaoxiang Sun6, Zhiyong Mao6, Houwen Lin7, Mingzhe Xiao2, Y Eugene Chin2, Hualiang Jiang5, Ying Xu8, Guoqiang Chen9, Jian Zhang10,11,12.
Abstract
SIRT6, a member of the SIRT deacetylase family, is responsible for deacetylation of histone H3 Nε-acetyl-lysines 9 (H3K9ac) and 56 (H3K56ac). As a tumor suppressor, SIRT6 has frequently been found to have low expression in various cancers. Here, we report the identification of MDL-800, a selective SIRT6 activator. MDL-800 increased the deacetylase activity of SIRT6 by up to 22-fold via binding to an allosteric site; this interaction led to a global decrease in H3K9ac and H3K56ac levels in human hepatocellular carcinoma (HCC) cells. Consequently, MDL-800 inhibited the proliferation of HCC cells via SIRT6-driven cell-cycle arrest and was effective in a tumor xenograft model. Together, these data demonstrate that pharmacological activation of SIRT6 is a potential therapeutic approach for the treatment of HCC. MDL-800 is a first-in-class small-molecule cellular SIRT6 activator that can be used to physiologically and pathologically investigate the roles of SIRT6 deacetylation.Entities:
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Year: 2018 PMID: 30374165 DOI: 10.1038/s41589-018-0150-0
Source DB: PubMed Journal: Nat Chem Biol ISSN: 1552-4450 Impact factor: 15.040