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核小体和转录谱摘要揭示了染色质结构和转录的决定因素。

A compendium of nucleosome and transcript profiles reveals determinants of chromatin architecture and transcription.

机构信息

Department of Genetics and Genomic Sciences, Icahn School of Medicine at Mount Sinai, New York, New York, United States of America.

出版信息

PLoS Genet. 2013 May;9(5):e1003479. doi: 10.1371/journal.pgen.1003479. Epub 2013 May 2.

Abstract

Nucleosomes in all eukaryotes examined to date adopt a characteristic architecture within genes and play fundamental roles in regulating transcription, yet the identity and precise roles of many of the trans-acting factors responsible for the establishment and maintenance of this organization remain to be identified. We profiled a compendium of 50 yeast strains carrying conditional alleles or complete deletions of genes involved in transcriptional regulation, histone biology, and chromatin remodeling, as well as compounds that target transcription and histone deacetylases, to assess their respective roles in nucleosome positioning and transcription. We find that nucleosome patterning in genes is affected by many factors, including the CAF-1 complex, Spt10, and Spt21, in addition to previously reported remodeler ATPases and histone chaperones. Disruption of these factors or reductions in histone levels led genic nucleosomes to assume positions more consistent with their intrinsic sequence preferences, with pronounced and specific shifts of the +1 nucleosome relative to the transcription start site. These shifts of +1 nucleosomes appear to have functional consequences, as several affected genes in Ino80 mutants exhibited altered expression responses. Our parallel expression profiling compendium revealed extensive transcription changes in intergenic and antisense regions, most of which occur in regions with altered nucleosome occupancy and positioning. We show that the nucleosome-excluding transcription factors Reb1, Abf1, Tbf1, and Rsc3 suppress cryptic transcripts at their target promoters, while a combined analysis of nucleosome and expression profiles identified 36 novel transcripts that are normally repressed by Tup1/Cyc8. Our data confirm and extend the roles of chromatin remodelers and chaperones as major determinants of genic nucleosome positioning, and these data provide a valuable resource for future studies.

摘要

迄今为止,所有已研究的真核生物中的核小体都采用了一种特征性的结构,在调节转录中发挥着基本作用,但负责建立和维持这种组织的许多反式作用因子的身份和确切作用仍有待确定。我们对一组 50 株酵母菌株进行了分析,这些菌株携带参与转录调控、组蛋白生物学和染色质重塑的条件等位基因或完全缺失,以及靶向转录和组蛋白去乙酰化酶的化合物,以评估它们在核小体定位和转录中的各自作用。我们发现,核小体在基因中的模式受到许多因素的影响,包括 CAF-1 复合物、Spt10 和 Spt21,以及以前报道的重塑 ATP 酶和组蛋白伴侣。这些因素的破坏或组蛋白水平的降低导致基因核小体占据更符合其内在序列偏好的位置,+1 核小体相对于转录起始位点的位置发生明显而特定的移动。这些+1 核小体的移动似乎具有功能后果,因为 Ino80 突变体中的几个受影响的基因表现出改变的表达反应。我们的平行表达谱综合分析揭示了基因间和反义区域的广泛转录变化,其中大多数发生在核小体占据和定位改变的区域。我们表明,排斥核小体的转录因子 Reb1、Abf1、Tbf1 和 Rsc3 在其靶启动子处抑制隐蔽转录物,而核小体和表达谱的综合分析确定了 36 个新的转录本,它们通常被 Tup1/Cyc8 抑制。我们的数据证实并扩展了染色质重塑因子和伴侣作为基因核小体定位主要决定因素的作用,这些数据为未来的研究提供了有价值的资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ebd0/3642058/09ea4579c0eb/pgen.1003479.g001.jpg

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