Literature DB >> 34159315

Accurate prediction of cis-regulatory modules reveals a prevalent regulatory genome of humans.

Pengyu Ni1, Zhengchang Su1.   

Abstract

cis-regulatory modules(CRMs) formed by clusters of transcription factor (TF) binding sites (TFBSs) are as important as coding sequences in specifying phenotypes of humans. It is essential to categorize all CRMs and constituent TFBSs in the genome. In contrast to most existing methods that predict CRMs in specific cell types using epigenetic marks, we predict a largely cell type agonistic but more comprehensive map of CRMs and constituent TFBSs in the gnome by integrating all available TF ChIP-seq datasets. Our method is able to partition 77.47% of genome regions covered by available 6092 datasets into a CRM candidate (CRMC) set (56.84%) and a non-CRMC set (43.16%). Intriguingly, the predicted CRMCs are under strong evolutionary constraints, while the non-CRMCs are largely selectively neutral, strongly suggesting that the CRMCs are likely cis-regulatory, while the non-CRMCs are not. Our predicted CRMs are under stronger evolutionary constraints than three state-of-the-art predictions (GeneHancer, EnhancerAtlas and ENCODE phase 3) and substantially outperform them for recalling VISTA enhancers and non-coding ClinVar variants. We estimated that the human genome might encode about 1.47M CRMs and 68M TFBSs, comprising about 55% and 22% of the genome, respectively; for both of which, we predicted 80%. Therefore, the cis-regulatory genome appears to be more prevalent than originally thought.
© The Author(s) 2021. Published by Oxford University Press on behalf of NAR Genomics and Bioinformatics.

Entities:  

Year:  2021        PMID: 34159315      PMCID: PMC8210889          DOI: 10.1093/nargab/lqab052

Source DB:  PubMed          Journal:  NAR Genom Bioinform        ISSN: 2631-9268


  135 in total

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Journal:  Database (Oxford)       Date:  2017-01-01       Impact factor: 3.451

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Authors:  Răzvan V Chereji; Peter R Eriksson; Josefina Ocampo; Hemant K Prajapati; David J Clark
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7.  UCNEbase--a database of ultraconserved non-coding elements and genomic regulatory blocks.

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9.  High-Resolution Epigenomic Atlas of Human Embryonic Craniofacial Development.

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10.  Exploiting regulatory heterogeneity to systematically identify enhancers with high accuracy.

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