Mediator Subunit Med4 Enforces Metastatic Dormancy in Breast Cancer.

Seong-Yeon Bae, Hsiang-Hsi Ling, Yi Chen, Hong Chen, Dhiraj Kumar, Jiankang Zhang, Aaron D Viny, Ronald A DePinho, Filippo G Giancotti
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Abstract

Long term survival of breast cancer patients is limited due to recurrence from metastatic dormant cancer cells. However, the mechanisms by which these dormant breast cancer cells survive and awaken remain poorly understood. Our unbiased genome-scale genetic screen in mice identified Med4 as a novel cancer-cell intrinsic gatekeeper in metastatic reactivation. MED4 haploinsufficiency is prevalent in metastatic breast cancer patients and correlates with poorer prognosis. Syngeneic xenograft models revealed that Med4 enforces breast cancer dormancy. Contrary to the canonical function of the Mediator complex in activating gene expression, Med4 maintains 3D chromatin compaction and enhancer landscape, by preventing enhancer priming or activation through the suppression of H3K4me1 deposition. Med4 haploinsufficiency disrupts enhancer poise and reprograms the enhancer dynamics to facilitate extracellular matrix (ECM) gene expression and integrin-mediated mechano-transduction, driving metastatic growth. Our findings establish Med4 as a key regulator of cellular dormancy and a potential biomarker for high-risk metastatic relapse.

通过整合素信号的表观遗传控制,Med4作为转移的守门人的非典型活性。
乳腺癌转移性复发后有一段潜伏期,称为转移性休眠期。通过在小鼠中进行遗传筛选,我们发现介质复合体亚基4 (Med4)在转移性再激活中是一种新的肿瘤细胞内在守门人。Med4下调有效地唤醒了休眠的乳腺癌细胞,促进了肺部的宏观转移性生长。与中介体的典型功能相反,Med4耗竭导致核大小和三维染色质结构从紧致状态到松弛状态的深刻变化。这些变化重新连接了细胞外基质蛋白、整合素和信号元件的表达,导致整合素介导的机械转导和YAP和MRTF的激活。应力纤维的组装拉动核膜,并有助于通过Med4耗竭加强整体染色质修饰。在转移性乳腺癌患者中观察到MED4基因缺失,并且MED4表达降低与预后不良相关,突出了其作为复发潜在生物标志物的重要性。意义:这项工作首次建立了Med4与其作为ECM程序的表观遗传和转录抑制因子的作用之间的联系,ECM程序在乳腺癌转移中重新激活休眠肿瘤细胞。我们强调了Med4与Med1不同的非规范作用,以及在体外和体内的功能意义。我们已经从功能上验证了通过遗传添加和化学抑制激活的异常信号通路,并将我们的发现与Med4表达、转移潜力和回顾性患者队列的总体结果联系起来。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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