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远距离转录因子结合位点聚集区域可能通过早期人类胚胎中的相分离相互作用介导转录调控。

Long-range transcription factor binding sites clustered regions may mediate transcriptional regulation through phase-separation interactions in early human embryo.

作者信息

Tian Mengge, Tang Xiaohan, Ouyang Zhangyi, Li Yaru, Bai Xuemei, Chen Bijia, Yue Shutong, Hu Pengzhen, Bo Xiaochen, Ren Chao, Chen Hebing, Lu Meisong

机构信息

The First Affiliated Hospital of Harbin Medical University, Harbin 150001, China.

Academy of Military Medical Sciences, Beijing 100850, China.

出版信息

Comput Struct Biotechnol J. 2024 Sep 26;23:3514-3526. doi: 10.1016/j.csbj.2024.09.017. eCollection 2024 Dec.

Abstract

In mammals, during the post-fertilization pre-implantation phase, the expression of cell type-specific genes is crucial for normal embryonic development, which is regulated by cis-regulatory elements (CREs). TFs control gene expression by interacting with CREs. Research shows that transcription factor binding sites (TFBSs) reflect the general characteristics of the regulatory genome. Here, we identified TFBSs from chromatin accessibility data in five stages of early human embryonic development, and quantified transcription factor binding sites-clustered regions (TFCRs) and their complexity (TC). Assigning TC values to TFCRs has made it possible to assess the functionality of these regulatory elements in a more quantitative way. Our findings reveal a robust correlation between TFCR complexity and gene expression starting from the 8Cell stage, which is when the zygotic genome is activated in humans. Furthermore, we have defined long-range TFCRs (LR-TFCRs) and conjecture that LR-TFCRs may regulate gene expression through phase-separation mechanisms during the early stages of human embryonic development.

摘要

在哺乳动物中,受精后的植入前阶段,细胞类型特异性基因的表达对于正常胚胎发育至关重要,这一过程由顺式调控元件(CREs)调控。转录因子(TFs)通过与CREs相互作用来控制基因表达。研究表明,转录因子结合位点(TFBSs)反映了调控基因组的一般特征。在此,我们从人类早期胚胎发育五个阶段的染色质可及性数据中鉴定出TFBSs,并对转录因子结合位点聚集区域(TFCRs)及其复杂性(TC)进行了量化。为TFCRs赋予TC值使得以更定量的方式评估这些调控元件的功能成为可能。我们的研究结果揭示了从8细胞阶段开始TFCR复杂性与基因表达之间的强烈相关性,8细胞阶段是人类合子基因组被激活的时期。此外,我们定义了长程TFCRs(LR-TFCRs),并推测LR-TFCRs可能在人类胚胎发育早期通过相分离机制调控基因表达。

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