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酿酒酵母基因组中由NuA4介导的染色质相关活动

NuA4-directed chromatin transactions throughout the Saccharomyces cerevisiae genome.

作者信息

Durant Melissa, Pugh B Franklin

机构信息

Center for Gene Regulation, Department of Biochemistry and Molecular Biology, The Pennsylvania State University, University Park, PA 16802, USA.

出版信息

Mol Cell Biol. 2007 Aug;27(15):5327-35. doi: 10.1128/MCB.00468-07. Epub 2007 May 25.

Abstract

Two of the major histone acetyltransferases in Saccharomyces cerevisiae are NuA4 and SAGA, which acetylate histones H4 and H3, respectively. Acetylated H3 and H4 tails have been implicated in binding bromodomain proteins, including Bdf1. Bdf1 interacts with the general transcription factor TFIID, which might promote preinitiation complex (PIC) assembly. Bdf1 also interacts with the SWR complex (SWR-C). SWR-C is responsible for the deposition of the histone H2A variant H2A.Z. The placement of these interactions into a connected pathway of PIC assembly has not been fully established. Moreover, it is not known how widespread and how variable such a pathway might be on a genomic scale. Here we provide genomic evidence for S. cerevisiae that PIC assembly (TFIID occupancy) and chromatin remodeling (SWR-C and H2A.Z occupancy) are linked in large part to NuA4-directed H4 acetylation and subsequent Bdf1 binding, rather than through SAGA-directed H3 acetylation. Bdf1 and its homolog Bdf2 tend to have distinct locations in the genome. However, the deletion of BDF1 leads to the accumulation of Bdf2 at Bdf1-vacated sites. Thus, while Bdf1 and Bdf2 are at least partially redundant in function, their functions in the genome are geographically distinct.

摘要

酿酒酵母中的两种主要组蛋白乙酰转移酶是NuA4和SAGA,它们分别使组蛋白H4和H3发生乙酰化。乙酰化的H3和H4尾部与包括Bdf1在内的含溴结构域蛋白的结合有关。Bdf1与通用转录因子TFIID相互作用,这可能会促进起始前复合物(PIC)的组装。Bdf1还与SWR复合物(SWR-C)相互作用。SWR-C负责组蛋白H2A变体H2A.Z的沉积。这些相互作用在PIC组装的连接途径中的位置尚未完全确定。此外,尚不清楚这样的途径在基因组规模上的广泛程度和可变程度如何。在这里,我们为酿酒酵母提供了基因组证据,表明PIC组装(TFIID占据)和染色质重塑(SWR-C和H2A.Z占据)在很大程度上与NuA4介导的H4乙酰化以及随后的Bdf1结合相关联,而不是通过SAGA介导的H3乙酰化。Bdf1及其同源物Bdf2在基因组中往往具有不同的位置。然而,BDF1的缺失会导致Bdf2在Bdf1 vacated位点积累。因此,虽然Bdf1和Bdf2在功能上至少部分冗余,但它们在基因组中的功能在空间上是不同的。

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