| Literature DB >> 31747604 |
Makoto Yamagishi1, Makoto Hori2, Dai Fujikawa3, Takeo Ohsugi4, Daisuke Honma5, Nobuaki Adachi6, Harutaka Katano7, Tsunekazu Hishima8, Seiichiro Kobayashi9, Kazumi Nakano2, Makoto Nakashima2, Masako Iwanaga10, Atae Utsunomiya11, Yuetsu Tanaka12, Seiji Okada13, Kunihiro Tsukasaki14, Kensei Tobinai15, Kazushi Araki16, Toshiki Watanabe17, Kaoru Uchimaru18.
Abstract
Although global H3K27me3 reprogramming is a hallmark of cancer, no effective therapeutic strategy for H3K27me3-high malignancies harboring EZH2WT/WT has yet been established. We explore epigenome and transcriptome in EZH2WT/WT and EZH2WT/Mu aggressive lymphomas and show that mutual interference and compensatory function of co-expressed EZH1 and EZH2 rearrange their own genome-wide distribution, thereby establishing restricted chromatin and gene expression signatures. Direct comparison of leading compounds introduces potency and a mechanism of action of the EZH1/2 dual inhibitor (valemetostat). The synthetic lethality is observed in all lymphoma models and primary adult T cell leukemia-lymphoma (ATL) cells. Opposing actions of EZH1/2-polycomb and SWI/SNF complexes are required for facultative heterochromatin formation. Inactivation of chromatin-associated genes (ARID1A, SMARCA4/BRG1, SMARCB1/SNF5, KDM6A/UTX, BAP1, KMT2D/MLL2) and oncovirus infection (HTLV-1, EBV) trigger EZH1/2 perturbation and H3K27me3 deposition. Our study provides the mechanism-based rationale for chemical dual targeting of EZH1/2 in cancer epigenome.Entities:
Keywords: EZH1; EZH2; H3K27me3; HTLV-1; adult T cell leukemia-lymphoma (ATL); epigenetic drug; malignant lymphoma; polycomb
Year: 2019 PMID: 31747604 DOI: 10.1016/j.celrep.2019.10.083
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423