Locus-specific proteomics identifies new aspects of the chromatin context involved in V region somatic hypermutation
Locus-specific proteomics identifies new aspects of the chromatin context involved in V region somatic hypermutation
Activation-induced cytidine deaminase (AID) somatically hypermutates the immunoglobulin heavy chain variable region (IGHV) gene to create the antibody diversity required to resist infections. This hypermutational process involves many pathways including transcription, DNA structural change and repair. While many of the proteins involved have been identified, their relative abundance, organization and regulation have not been resolved and additional factors and pathways need to be identified. To identify the proteome occupying IGHV, we have utilized dCas9-APEX targeted by guide RNAs to biotinylate and enrich the proteins associated with the mutating V region chromatin in the Ramos human B cell line and compared them to the non-mutating downstream constant region (C) chromatin. We identified hundreds of proteins specifically enriched on the V or C region. We confirmed the functionality of selected factors by examining the changes in the V region-specific proteome after inhibiting transcriptional elongation and somatic mutation with the Dot1L inhibitor EPZ004777.
Yu GuoYun、Zhang Yongwei、Aguilan Jennifer、Duan Zhi、Scharff Matthew D、Sidoli Simone
基础医学生物科学研究方法、生物科学研究技术分子生物学
Yu GuoYun,Zhang Yongwei,Aguilan Jennifer,Duan Zhi,Scharff Matthew D,Sidoli Simone.Locus-specific proteomics identifies new aspects of the chromatin context involved in V region somatic hypermutation[EB/OL].(2025-03-28)[2025-04-24].https://www.biorxiv.org/content/10.1101/2022.09.08.507190.点此复制
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