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米托蒽醌诱导横纹肌瘤的启动子重编程和分化。

Mithramycin induces promoter reprogramming and differentiation of rhabdoid tumor.

机构信息

Van Andel Research Institute, Grand Rapids, MI, USA.

Dartmouth College, Hanover, NH, USA.

出版信息

EMBO Mol Med. 2021 Feb 5;13(2):e12640. doi: 10.15252/emmm.202012640. Epub 2020 Dec 17.

Abstract

Rhabdoid tumor (RT) is a pediatric cancer characterized by the inactivation of SMARCB1, a subunit of the SWI/SNF chromatin remodeling complex. Although this deletion is the known oncogenic driver, there are limited effective therapeutic options for these patients. Here we use unbiased screening of cell line panels to identify a heightened sensitivity of rhabdoid tumor to mithramycin and the second-generation analogue EC8042. The sensitivity of MMA and EC8042 was superior to traditional DNA damaging agents and linked to the causative mutation of the tumor, SMARCB1 deletion. Mithramycin blocks SMARCB1-deficient SWI/SNF activity and displaces the complex from chromatin to cause an increase in H3K27me3. This triggers chromatin remodeling and enrichment of H3K27ac at chromHMM-defined promoters to restore cellular differentiation. These effects occurred at concentrations not associated with DNA damage and were not due to global chromatin remodeling or widespread gene expression changes. Importantly, a single 3-day infusion of EC8042 caused dramatic regressions of RT xenografts, recapitulated the increase in H3K27me3, and cellular differentiation described in vitro to completely cure three out of eight mice.

摘要

横纹肌瘤(RT)是一种儿科癌症,其特征是 SMARCB1 的失活,SMARCB1 是 SWI/SNF 染色质重塑复合物的一个亚基。尽管这种缺失是已知的致癌驱动因素,但这些患者的有效治疗选择有限。在这里,我们使用无偏筛选细胞系面板来鉴定横纹肌瘤对米托蒽醌和第二代类似物 EC8042 的敏感性增加。MMA 和 EC8042 的敏感性优于传统的 DNA 损伤剂,并与肿瘤的致病突变 SMARCB1 缺失有关。米托蒽醌阻断 SMARCB1 缺陷型 SWI/SNF 活性,并将复合物从染色质上置换下来,导致 H3K27me3 增加。这引发了染色质重塑和 H3K27ac 在 chromHMM 定义的启动子处的富集,以恢复细胞分化。这些效应发生在与 DNA 损伤无关的浓度下,并且不是由于全局染色质重塑或广泛的基因表达变化引起的。重要的是,单次 3 天的 EC8042 输注导致 RT 异种移植物的显著消退,重现了体外描述的 H3K27me3 增加和细胞分化,从而完全治愈了 8 只小鼠中的 3 只。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4df/7863405/03f9b333fbdf/EMMM-13-e12640-g002.jpg

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