| Literature DB >> 30220457 |
Xun Huang1, Juan Yan2, Min Zhang3, Yafang Wang1, Yi Chen1, Xuhong Fu1, Rongrui Wei1, Xing-Ling Zheng2, Zhiwei Liu3, Xiong Zhang1, Hong Yang1, Bingbing Hao4, Yan-Yan Shen1, Yi Su1, Xiaoji Cong3, Min Huang1, Minjia Tan5, Jian Ding6, Meiyu Geng7.
Abstract
Mutations or aberrant upregulation of EZH2 occur frequently in human cancers, yet clinical benefits of EZH2 inhibitor (EZH2i) remain unsatisfactory and limited to certain hematological malignancies. We profile global posttranslational histone modification changes across a large panel of cancer cell lines with various sensitivities to EZH2i. We report here oncogenic transcriptional reprogramming mediated by MLL1's interaction with the p300/CBP complex, which directs H3K27me loss to reciprocal H3K27ac gain and restricts EZH2i response. Concurrent inhibition of H3K27me and H3K27ac results in transcriptional repression and MAPK pathway dependency in cancer subsets. In preclinical models encompassing a broad spectrum of EZH2-aberrant solid tumors, a combination of EZH2 and BRD4 inhibitors, or a triple-combination including MAPK inhibition display robust efficacy with very tolerable toxicity. Our results suggest an attractive precision treatment strategy for EZH2-aberrant tumors on the basis of tumor-intrinsic MLL1 expression and concurrent inhibition of epigenetic crosstalk and feedback MAPK activation.Entities:
Keywords: EZH2; H3K27; MAPK; MLL1; acetylation; cancer; crosstalk; histone; methylation; therapy
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Year: 2018 PMID: 30220457 DOI: 10.1016/j.cell.2018.08.058
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582