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转录激活因子将组蛋白乙酰转移酶复合物导向核小体。

Transcriptional activators direct histone acetyltransferase complexes to nucleosomes.

作者信息

Utley R T, Ikeda K, Grant P A, Côté J, Steger D J, Eberharter A, John S, Workman J L

机构信息

Howard Hughes Medical Institute, Department of Biochemistry and Molecular Biology, Pennsylvania State University, University Park 16802-4500, USA.

出版信息

Nature. 1998 Jul 30;394(6692):498-502. doi: 10.1038/28886.

Abstract

Transcriptional co-activators were originally identified as proteins that act as intermediaries between upstream activators and the basal transcription machinery. The discovery that co-activators such as Tetrahymena and yeast Gcn5, as well as human p300/CBP, pCAF, Src-1, ACTR and TAFII250, can acetylate histones suggests that activators may be involved in targeting acetylation activity to promoters. Several histone deacetylases have been linked to transcriptional co-repressor proteins, suggesting that the action of both acetylases and deacetylases is important in the regulation of many genes. Here we demonstrate the binding of two native yeast histone acetyltransferase (HAT) complexes to the herpesvirus VP16 activation domain and the yeast transcriptional activator Gcn4, and show that it is their interaction with the VP16 activation domain that targets Gal4-VP16-bound nucleosomes for acetylation. We find that Gal4-VP16-driven transcription from chromatin templates is stimulated by both HAT complexes in an acetyl CoA-dependent reaction. Our results demonstrate the targeting of native HAT complexes by a transcription-activation domain to nucleosomes in order to activate transcription.

摘要

转录共激活因子最初被鉴定为在上游激活因子和基础转录机制之间起中介作用的蛋白质。诸如四膜虫和酵母Gcn5以及人类p300/CBP、pCAF、Src-1、ACTR和TAFII250等共激活因子能够使组蛋白乙酰化,这一发现表明激活因子可能参与将乙酰化活性靶向启动子。几种组蛋白去乙酰化酶已与转录共抑制蛋白相关联,这表明乙酰化酶和去乙酰化酶的作用在许多基因的调控中都很重要。在这里,我们证明了两种天然酵母组蛋白乙酰转移酶(HAT)复合物与疱疹病毒VP16激活域和酵母转录激活因子Gcn4的结合,并表明正是它们与VP16激活域的相互作用将与Gal4-VP16结合的核小体靶向进行乙酰化。我们发现,两种HAT复合物在依赖于乙酰辅酶A的反应中均能刺激染色质模板上由Gal4-VP16驱动的转录。我们的结果证明了转录激活域将天然HAT复合物靶向核小体以激活转录。

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