ZNF143 provides sequence specificity to secure chromatin interactions at gene promoters

ZNF143 提供序列特异性以确保基因启动子处的染色质相互作用

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作者:Swneke D Bailey, Xiaoyang Zhang, Kinjal Desai, Malika Aid, Olivia Corradin, Richard Cowper-Sal Lari, Batool Akhtar-Zaidi, Peter C Scacheri, Benjamin Haibe-Kains, Mathieu Lupien

Abstract

Chromatin interactions connect distal regulatory elements to target gene promoters guiding stimulus- and lineage-specific transcription. Few factors securing chromatin interactions have so far been identified. Here, by integrating chromatin interaction maps with the large collection of transcription factor-binding profiles provided by the ENCODE project, we demonstrate that the zinc-finger protein ZNF143 preferentially occupies anchors of chromatin interactions connecting promoters with distal regulatory elements. It binds directly to promoters and associates with lineage-specific chromatin interactions and gene expression. Silencing ZNF143 or modulating its DNA-binding affinity using single-nucleotide polymorphisms (SNPs) as a surrogate of site-directed mutagenesis reveals the sequence dependency of chromatin interactions at gene promoters. We also find that chromatin interactions alone do not regulate gene expression. Together, our results identify ZNF143 as a novel chromatin-looping factor that contributes to the architectural foundation of the genome by providing sequence specificity at promoters connected with distal regulatory elements.

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