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高核小体占有率被编码在人类调控序列中。

High nucleosome occupancy is encoded at human regulatory sequences.

机构信息

Department of Molecular Genetics, University of Toronto, Toronto, Canada.

出版信息

PLoS One. 2010 Feb 9;5(2):e9129. doi: 10.1371/journal.pone.0009129.

Abstract

Active eukaryotic regulatory sites are characterized by open chromatin, and yeast promoters and transcription factor binding sites (TFBSs) typically have low intrinsic nucleosome occupancy. Here, we show that in contrast to yeast, DNA at human promoters, enhancers, and TFBSs generally encodes high intrinsic nucleosome occupancy. In most cases we examined, these elements also have high experimentally measured nucleosome occupancy in vivo. These regions typically have high G+C content, which correlates positively with intrinsic nucleosome occupancy, and are depleted for nucleosome-excluding poly-A sequences. We propose that high nucleosome preference is directly encoded at regulatory sequences in the human genome to restrict access to regulatory information that will ultimately be utilized in only a subset of differentiated cells.

摘要

活性真核调控位点的特征是开放染色质,而酵母启动子和转录因子结合位点 (TFBS) 通常具有较低的固有核小体占有率。在这里,我们表明与酵母相反,人类启动子、增强子和 TFBS 中的 DNA 通常编码高固有核小体占有率。在我们检查的大多数情况下,这些元件在体内也具有高实验测量的核小体占有率。这些区域通常具有高 GC 含量,这与固有核小体占有率呈正相关,并且缺乏排除核小体的多 A 序列。我们提出,高核小体偏好直接编码在人类基因组的调控序列中,以限制对调控信息的访问,这些信息最终仅在一部分分化细胞中使用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/89a4/2817738/6c239e026794/pone.0009129.g001.jpg

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