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由COMPASS介导的H2B单泛素化与H3甲基化之间的组蛋白串扰。

Histone crosstalk between H2B monoubiquitination and H3 methylation mediated by COMPASS.

作者信息

Lee Jung-Shin, Shukla Abhijit, Schneider Jessica, Swanson Selene K, Washburn Michael P, Florens Laurence, Bhaumik Sukesh R, Shilatifard Ali

机构信息

Stowers Institute for Medical Research, 1000 East 50(th) Street, Kansas City, MO 64110, USA.

出版信息

Cell. 2007 Dec 14;131(6):1084-96. doi: 10.1016/j.cell.2007.09.046.

Abstract

COMPASS, the yeast homolog of the mammalian MLL complex, is a histone H3 lysine 4 (H3K4) methylase consisting of Set1 (KMT2) and seven other polypeptides, including Cps35, the only essential subunit. Histone H2B monoubiquitination by Rad6/Bre1 is required for both H3K4 methylation by COMPASS, and H3K79 methylation by Dot1. However, the molecular mechanism for such histone crosstalk is poorly understood. Here, we demonstrate that histone H2B monoubiquitination controls the binding of Cps35 with COMPASS complex. Cps 35 is required for COMPASS' catalytic activity in vivo, and the addition of exogenous purified Cps35 to COMPASS purified from a Deltarad6 background results in the generation of a methylation competent COMPASS. Cps35 associates with the chromatin of COMPASS-regulated genes in a H2BK123 monoubiquitination-dependent but Set1-independent manner. Cps35 is also required for proper H3K79 trimethylation. These findings offer insight into the molecular role of Cps35 in translating the H2B monoubiquitination signal into H3 methylation.

摘要

COMPASS是哺乳动物MLL复合物的酵母同源物,是一种组蛋白H3赖氨酸4(H3K4)甲基转移酶,由Set1(KMT2)和其他七种多肽组成,包括唯一必需的亚基Cps35。Rad6/Bre1介导的组蛋白H2B单泛素化对于COMPASS介导的H3K4甲基化和Dot1介导的H3K79甲基化都是必需的。然而,这种组蛋白相互作用的分子机制尚不清楚。在这里,我们证明组蛋白H2B单泛素化控制Cps35与COMPASS复合物的结合。Cps35是COMPASS在体内催化活性所必需的,将外源纯化的Cps35添加到从Deltarad6背景纯化的COMPASS中会导致产生具有甲基化活性的COMPASS。Cps35以H2BK123单泛素化依赖性但Set1非依赖性的方式与COMPASS调控基因的染色质结合。Cps35对于正确的H3K79三甲基化也是必需的。这些发现为Cps35在将H2B单泛素化信号转化为H3甲基化中的分子作用提供了见解。

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