复制体近端蛋白关联和停滞复制叉的动态蛋白质组变化

IF 6.1 2区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS Molecular & Cellular Proteomics Pub Date : 2024-05-01 Epub Date: 2024-04-13 DOI:10.1016/j.mcpro.2024.100767
Carla-Marie Jurkovic, Jennifer Raisch, Stephanie Tran, Hoang Dong Nguyen, Dominique Lévesque, Michelle S Scott, Eric I Campos, François-Michel Boisvert
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引用次数: 0

摘要

DNA 复制是细胞分裂过程中确保遗传信息传递的基本细胞过程。基因组复制发生在 S 期,需要在复制叉上动态、高度协调地招募多种蛋白质。各种基因毒性应激源会导致分叉不稳定和崩溃,因此需要 DNA 修复途径。通过识别这些事件中涉及的多种蛋白质相互作用,我们可以更好地掌握促进 DNA 复制和修复的复杂而动态的分子机制。我们利用亲近依赖性生物素鉴定(BioID)技术鉴定了四种核心复制元件中 17 种蛋白质的关联,这四种核心复制元件分别是拆分 DNA 的 CDC45/MCM2-7/GINS (CMG) 螺旋酶、DNA 聚合酶、复制蛋白 A 亚基以及拆分和重新组装染色质所需的组蛋白伴侣。我们进一步研究了基因毒性应激对这些相互作用的影响。这项分析表明,在羟基脲存在的情况下,有108个核蛋白进一步调节了庞大的邻近关联网络;其中45个核蛋白富集,63个核蛋白减少。有趣的是,羟基脲处理还导致与 11 个相互作用者的关联重新分布,这意味着复制体在受压时会发生动态重组。这项分析发现了几种特征不清的蛋白质,从而揭示了细胞对 DNA 复制停滞反应的新的假定参与者。它还提供了一个新的综合蛋白质组框架,以了解细胞如何应对 DNA 复制过程中的障碍。
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Replisome Proximal Protein Associations and Dynamic Proteomic Changes at Stalled Replication Forks.

DNA replication is a fundamental cellular process that ensures the transfer of genetic information during cell division. Genome duplication takes place in S phase and requires a dynamic and highly coordinated recruitment of multiple proteins at replication forks. Various genotoxic stressors lead to fork instability and collapse, hence the need for DNA repair pathways. By identifying the multitude of protein interactions implicated in those events, we can better grasp the complex and dynamic molecular mechanisms that facilitate DNA replication and repair. Proximity-dependent biotin identification was used to identify associations with 17 proteins within four core replication components, namely the CDC45/MCM2-7/GINS helicase that unwinds DNA, the DNA polymerases, replication protein A subunits, and histone chaperones needed to disassemble and reassemble chromatin. We further investigated the impact of genotoxic stress on these interactions. This analysis revealed a vast proximity association network with 108 nuclear proteins further modulated in the presence of hydroxyurea; 45 being enriched and 63 depleted. Interestingly, hydroxyurea treatment also caused a redistribution of associations with 11 interactors, meaning that the replisome is dynamically reorganized when stressed. The analysis identified several poorly characterized proteins, thereby uncovering new putative players in the cellular response to DNA replication arrest. It also provides a new comprehensive proteomic framework to understand how cells respond to obstacles during DNA replication.

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来源期刊
Molecular & Cellular Proteomics
Molecular & Cellular Proteomics 生物-生化研究方法
CiteScore
11.50
自引率
4.30%
发文量
131
审稿时长
84 days
期刊介绍: The mission of MCP is to foster the development and applications of proteomics in both basic and translational research. MCP will publish manuscripts that report significant new biological or clinical discoveries underpinned by proteomic observations across all kingdoms of life. Manuscripts must define the biological roles played by the proteins investigated or their mechanisms of action. The journal also emphasizes articles that describe innovative new computational methods and technological advancements that will enable future discoveries. Manuscripts describing such approaches do not have to include a solution to a biological problem, but must demonstrate that the technology works as described, is reproducible and is appropriate to uncover yet unknown protein/proteome function or properties using relevant model systems or publicly available data. Scope: -Fundamental studies in biology, including integrative "omics" studies, that provide mechanistic insights -Novel experimental and computational technologies -Proteogenomic data integration and analysis that enable greater understanding of physiology and disease processes -Pathway and network analyses of signaling that focus on the roles of post-translational modifications -Studies of proteome dynamics and quality controls, and their roles in disease -Studies of evolutionary processes effecting proteome dynamics, quality and regulation -Chemical proteomics, including mechanisms of drug action -Proteomics of the immune system and antigen presentation/recognition -Microbiome proteomics, host-microbe and host-pathogen interactions, and their roles in health and disease -Clinical and translational studies of human diseases -Metabolomics to understand functional connections between genes, proteins and phenotypes
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