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DNA灵活性调节转录因子与核小体的结合。

DNA flexibility regulates transcription factor binding to nucleosomes.

作者信息

Mariani Luca, Liu Xiao, Lee Kwangwoon, Gisselbrecht Stephen S, Cole Philip A, Bulyk Martha L

机构信息

Division of Genetics, Department of Medicine; Brigham and Women's Hospital and Harvard Medical School, Boston, MA 02115.

Department of Biomedical Informatics; Harvard Medical School, Boston, MA 02115.

出版信息

bioRxiv. 2024 Sep 2:2024.09.02.610559. doi: 10.1101/2024.09.02.610559.

Abstract

Cell fate decisions are controlled by sequence-specific transcription factors (TFs), referred to as 'pioneer' factors, that bind their target sites within nucleosomes ('pioneer binding') and thus initiate chromatin opening. However, pioneers bind just a minority of their recognition sequences present in the genome, suggesting that local sequence context features may regulate pioneer binding. Here, we developed PIONEAR-seq, a highly parallel sequencing-based biochemical assay for high-throughput analysis of TF binding to nucleosomes on nucleosome positioning sequences. Using PIONEAR-seq, we characterized the pioneer binding of 7 human pioneer TFs. Comparison of TF binding to nucleosomes based on the synthetic Widom 601 (W601) model sequence versus three different genomic sequences revealed that the positional preferences of these TFs' binding to nucleosomes (, dyad, periodic and end binding) is determined by the broader sequence context of the nucleosome, rather than being a property intrinsic to the TF. We propose a model where the flexibility and rigidity within nucleosomal DNA regulate where pioneers bind within nucleosomes. Our results suggest that the broader physical properties of nucleosomal DNA represent another layer of -regulatory information read out by TFs in eukaryotic genomes.

摘要

细胞命运决定由序列特异性转录因子(TFs)控制,这些转录因子被称为“先锋”因子,它们在核小体内结合其靶位点(“先锋结合”),从而启动染色质开放。然而,先锋因子仅结合基因组中少数其识别序列,这表明局部序列背景特征可能调节先锋结合。在此,我们开发了PIONEAR-seq,这是一种基于高度平行测序的生化分析方法,用于在核小体定位序列上高通量分析TF与核小体的结合。使用PIONEAR-seq,我们表征了7种人类先锋TF的先锋结合。基于合成的Widom 601(W601)模型序列与三种不同基因组序列比较TF与核小体的结合,结果显示这些TF与核小体结合的位置偏好(即二分体、周期性和末端结合)由核小体更广泛的序列背景决定,而非TF的固有特性。我们提出了一个模型,其中核小体DNA内的灵活性和刚性调节先锋因子在核小体内的结合位置。我们的结果表明,核小体DNA更广泛的物理特性代表了真核基因组中TF读取的另一层调控信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81cf/11507811/4966e24f76d3/nihpp-2024.09.02.610559v1-f0001.jpg

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