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组蛋白甲基转移酶的结构域识别 ISWI 重塑的核小体物种。

SET domains of histone methyltransferases recognize ISWI-remodeled nucleosomal species.

机构信息

Institute of Developmental Biology, Moscow 117334, Russian Federation.

出版信息

Mol Cell Biol. 2010 Feb;30(3):552-64. doi: 10.1128/MCB.00775-09. Epub 2009 Sep 14.

DOI:10.1128/MCB.00775-09
PMID:19752191
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2812232/
Abstract

The trithorax (trxG) and Polycomb (PcG) group proteins recognize and propagate inheritable patterns of gene expression through a poorly understood epigenetic mechanism. A distinguishing feature of these proteins is the presence of a 130-amino-acid methyltransferase domain (SET), which catalyzes the methylation of histones. It is still not clear how SET proteins distinguish gene expression states, how they are targeted, or what regulates their substrate specificity. Many SET domain-containing proteins show robust activity on core histones but relatively weak activity on intact nucleosomes, their physiological substrate. Here, we examined the binding of two SET domain-containing proteins, ALL1 and SET7, to chromatin substrates. The SET domains from these proteins bind and methylate intact nucleosomes poorly but can recognize disrupted nucleosomal structures associated with transcribed chromatin. Interestingly, the remodeling of dinucleosomes by the ISWI class of ATP-dependent chromatin remodeling enzymes stimulated the binding of SET domains to chromatin and the methylation of H3 within the nucleosome. Unexpectedly, dinucleosomes remodeled by SWI/SNF were poor substrates. Thus, SET domains can distinguish nucleosomes altered by these two classes of remodeling enzymes. Our study reveals novel insights into the mechanism of how SET domains recognize different chromatin states and specify histone methylation at active loci.

摘要

转录激活因子复合物相关蛋白(trxG)和 Polycomb(PcG)组蛋白通过一种尚未完全阐明的表观遗传机制识别和传播可遗传的基因表达模式。这些蛋白的一个显著特征是存在一个 130 个氨基酸的甲基转移酶结构域(SET),该结构域催化组蛋白的甲基化。目前尚不清楚 SET 蛋白如何区分基因表达状态,它们如何被靶向,或者什么调节它们的底物特异性。许多含有 SET 结构域的蛋白在核心组蛋白上表现出很强的活性,但在其生理底物完整核小体上的活性相对较弱。在这里,我们研究了两种含有 SET 结构域的蛋白 ALL1 和 SET7 与染色质底物的结合。这两种蛋白的 SET 结构域对完整核小体的结合和甲基化作用较弱,但能识别与转录相关的染色质中被破坏的核小体结构。有趣的是,由 ISWI 类 ATP 依赖的染色质重塑酶重塑的二核小体刺激了 SET 结构域与染色质的结合以及核小体中 H3 的甲基化。出乎意料的是,SWI/SNF 重塑的二核小体是较差的底物。因此,SET 结构域可以区分这两类重塑酶改变的核小体。我们的研究揭示了 SET 结构域如何识别不同染色质状态以及在活性基因座特异性组蛋白甲基化的新机制。

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