Department of Bionanoscience, Kavli Institute of Nanoscience, Delft University of Technology, Delft, The Netherlands.
Chromosome Replication Laboratory, Francis Crick Institute, London, UK.
Nat Commun. 2021 Mar 26;12(1):1908. doi: 10.1038/s41467-021-22216-x.
DNA replication in eukaryotes initiates at many origins distributed across each chromosome. Origins are bound by the origin recognition complex (ORC), which, with Cdc6 and Cdt1, recruits and loads the Mcm2-7 (MCM) helicase as an inactive double hexamer during G1 phase. The replisome assembles at the activated helicase in S phase. Although the outline of replisome assembly is understood, little is known about the dynamics of individual proteins on DNA and how these contribute to proper complex formation. Here we show, using single-molecule optical trapping and confocal microscopy, that yeast ORC is a mobile protein that diffuses rapidly along DNA. Origin recognition halts this search process. Recruitment of MCM molecules in an ORC- and Cdc6-dependent fashion results in slow-moving ORC-MCM intermediates and MCMs that rapidly scan the DNA. Following ATP hydrolysis, salt-stable loading of MCM single and double hexamers was seen, both of which exhibit salt-dependent mobility. Our results demonstrate that effective helicase loading relies on an interplay between protein diffusion and origin recognition, and suggest that MCM is stably loaded onto DNA in multiple forms.
真核生物中的 DNA 复制从分布在每条染色体上的多个起始点开始。起始点被起始识别复合物(ORC)所结合,ORC 与 Cdc6 和 Cdt1 一起在 G1 期招募并加载 Mcm2-7(MCM)解旋酶作为无活性的双六聚体。复制体在 S 期在激活的解旋酶处组装。尽管复制体组装的大致轮廓已经清楚,但对于 DNA 上单个蛋白质的动力学以及这些蛋白质如何有助于正确的复合物形成知之甚少。在这里,我们使用单分子光学俘获和共聚焦显微镜显示,酵母 ORC 是一种可在 DNA 上快速扩散的移动蛋白。起始识别阻止了这种搜索过程。以 ORC 和 Cdc6 依赖性的方式募集 MCM 分子会导致缓慢移动的 ORC-MCM 中间体和快速扫描 DNA 的 MCM。在 ATP 水解后,观察到 MCM 单六聚体和双六聚体的稳定加载,两者都表现出盐依赖性的迁移能力。我们的结果表明,有效的解旋酶加载依赖于蛋白扩散和起始识别之间的相互作用,并表明 MCM 以多种形式稳定地加载到 DNA 上。
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