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单碱基分辨率分析 DNA 结合基序与 Motif 揭示了 CTCF 锌指 1 突变的致癌功能。

Single base-pair resolution analysis of DNA binding motif with MoMotif reveals an oncogenic function of CTCF zinc-finger 1 mutation.

机构信息

Department of Experimental Medicine, McGill University, Montréal, Québec H3A 0G4, Canada.

Lady Davis Institute, Jewish General Hospital, Montréal, Québec H3T 1E2, Canada.

出版信息

Nucleic Acids Res. 2022 Aug 26;50(15):8441-8458. doi: 10.1093/nar/gkac658.

Abstract

Defining the impact of missense mutations on the recognition of DNA motifs is highly dependent on bioinformatic tools that define DNA binding elements. However, classical motif analysis tools remain limited in their capacity to identify subtle changes in complex binding motifs between distinct conditions. To overcome this limitation, we developed a new tool, MoMotif, that facilitates a sensitive identification, at the single base-pair resolution, of complex, or subtle, alterations to core binding motifs, discerned from ChIP-seq data. We employed MoMotif to define the previously uncharacterized recognition motif of CTCF zinc-finger 1 (ZF1), and to further define the impact of CTCF ZF1 mutation on its association with chromatin. Mutations of CTCF ZF1 are exclusive to breast cancer and are associated with metastasis and therapeutic resistance, but the underlying mechanisms are unclear. Using MoMotif, we identified an extension of the CTCF core binding motif, necessitating a functional ZF1 to bind appropriately. Using a combination of ChIP-Seq and RNA-Seq, we discover that the inability to bind this extended motif drives an altered transcriptional program associated with the oncogenic phenotypes observed clinically. Our study demonstrates that MoMotif is a powerful new tool for comparative ChIP-seq analysis and characterising DNA-protein contacts.

摘要

定义错义突变对 DNA 基序识别的影响高度依赖于定义 DNA 结合元件的生物信息学工具。然而,经典的基序分析工具在识别不同条件下复杂结合基序中的细微变化方面仍然存在局限性。为了克服这一限制,我们开发了一种新工具 MoMotif,该工具可以在单碱基分辨率下,灵敏地识别从 ChIP-seq 数据中推断出的核心结合基序的复杂或细微改变。我们利用 MoMotif 来定义 CTCF 锌指 1 (ZF1) 以前未被表征的识别基序,并进一步定义 CTCF ZF1 突变对其与染色质结合的影响。CTCF ZF1 的突变是乳腺癌所特有的,与转移和治疗耐药性有关,但潜在的机制尚不清楚。使用 MoMotif,我们确定了 CTCF 核心结合基序的扩展,需要功能齐全的 ZF1 才能正确结合。通过结合 ChIP-Seq 和 RNA-Seq,我们发现无法结合这个扩展的基序会导致与临床上观察到的致癌表型相关的转录程序发生改变。我们的研究表明,MoMotif 是一种用于比较 ChIP-seq 分析和表征 DNA-蛋白质相互作用的强大新工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c7c9/9410893/b08b58d627d1/gkac658fig1.jpg

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