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Insights into the Architecture of the Replicative Helicase from the Structure of an Archaeal MCM Homolog

机译:从古细菌MCM同源物的结构洞悉复制解旋酶的体系结构

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摘要

The minichromosome maintenance (MCM) proteins, members of the AAA+ (ATPase associated with diverse cellular activities) superfamily, are believed to constitute the replicative helicase in eukaryotic and archaeal species. Here, we present the 1.9 A resolution crystal structure of a monomeric MCM homolog from Methanopyrus kandleri, the first crystallographic structure of a full-length MCM. We also present an 18 angstrom cryo-electron microscopy reconstruction of the hexameric MCM from Methanothermobacter thermautotrophicus, and fit the atomic resolution crystal structure into the reconstruction in order to generate an atomic model for the oligomeric assembly. These structural data reveal a distinct active site topology consisting of a unique arrangement of critical determinants. The structures also provide a molecular framework for understanding the functional contributions of trans-acting elements that facilitate intersubunit crosstalk in response to DNA binding and ATP hydrolysis.
机译:AAA +(与多种细胞活动相关的ATPase)超家族成员的微染色体维持(MCM)蛋白被认为构成了真核和古细菌物种中的复制性解旋酶。在这里,我们介绍了来自Methanopyrus kandleri的单体MCM同系物的1.9 A分辨率晶体结构,这是全长MCM的第一个晶体结构。我们还提出了甲烷热解自甲烷甲烷杆菌的六聚体MCM的18埃低温电子显微镜重建,并将原子分辨率晶体结构纳入重建中,以便为低聚体组装生成原子模型。这些结构数据揭示了由关键决定因素的独特排列组成的独特的活动场所拓扑。该结构还提供了一个分子框架,用于理解反式作用元件的功能性贡献,这些作用元件促进亚单位间的串扰以响应DNA结合和ATP水解。

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