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由可解离激酶模块调节的人类转录中介体复合物的结构基础

Structural basis of the human transcriptional Mediator complex modulated by its dissociable Kinase module.

作者信息

Chen Shin-Fu, Chao Ti-Chun, Kim Hee Jong, Tang Hui-Chi, Khadka Subash, Li Tao, Lee Dung-Fang, Murakami Kenji, Boyer Thomas G, Tsai Kuang-Lei

出版信息

bioRxiv. 2024 Jul 3:2024.07.01.601608. doi: 10.1101/2024.07.01.601608.

Abstract

The eukaryotic Mediator, comprising a large Core (cMED) and a dissociable CDK8 kinase module (CKM), regulates RNA Polymerase II (Pol II)-dependent transcription. cMED recruits Pol II and promotes pre-initiation complex (PIC) formation in a manner inhibited by the CKM, which is also implicated in post-initiation control of gene expression. Herein we report cryo-electron microscopy structures of the human complete Mediator and its CKM, which explains the basis for CKM inhibition of cMED-activated transcription. The CKM binds to cMED through an intrinsically disordered region (IDR) in MED13 and HEAT repeats in MED12. The CKM inhibits transcription by allocating its MED13 IDR to occlude binding of Pol II and MED26 to cMED and further obstructing cMED-PIC assembly through steric hindrance with TFIIH and the +1 nucleosome. Notably, MED12 binds to the cMED Hook, positioning CDK8 downstream of the transcription start site, which sheds new light on its stimulatory function in post-initiation events.

摘要

真核生物中介体由一个大型核心(cMED)和一个可解离的CDK8激酶模块(CKM)组成,它调节RNA聚合酶II(Pol II)依赖性转录。cMED招募Pol II并以一种被CKM抑制的方式促进起始前复合物(PIC)的形成,CKM也参与基因表达的起始后控制。在此我们报告了人类完整中介体及其CKM的冷冻电子显微镜结构,这解释了CKM抑制cMED激活转录的基础。CKM通过MED13中的一个内在无序区域(IDR)和MED12中的HEAT重复序列与cMED结合。CKM通过分配其MED13 IDR来抑制转录,以阻断Pol II和MED26与cMED的结合,并通过与TFIIH和+1核小体的空间位阻进一步阻碍cMED-PIC组装。值得注意的是,MED12与cMED钩结合,将CDK8定位在转录起始位点的下游,这为其在起始后事件中的刺激功能提供了新的线索。

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