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具有多个微染色体维持基因的古菌目。

An archaeal order with multiple minichromosome maintenance genes.

机构信息

Department of Biology (Area 5), PO Box 373, University of York, York YO10 5YW, UK.

出版信息

Microbiology (Reading). 2010 May;156(Pt 5):1405-1414. doi: 10.1099/mic.0.036707-0. Epub 2010 Feb 4.

DOI:10.1099/mic.0.036707-0
PMID:20133362
Abstract

In eukaryotes, a complex of six highly related minichromosome maintenance (MCM) proteins is believed to function as the replicative helicase. Until recently, systems for exploring the molecular mechanisms underlying eukaryotic MCM function have been biochemically intractable. To overcome this, molecular studies of MCM function have been carried out using MCM homologues from the archaea. Archaeal MCM systems studied to date possess a single functional MCM, which forms a homohexameric complex that displays DNA binding, ATPase and helicase activities. We have identified an archaeal order that possesses multiple MCM homologues. blast searches of available Methanococcales genomes reveal that members of this order possess between two and eight MCM homologues. Phylogenetic analysis suggests that an ancient duplication in the Methanococcales gave rise to two major groups of MCMs. One group contains Methanococcus maripaludis S2 McmD and possesses a conserved C-terminal insert similar to one observed in eukaryotic MCM3, while the other group contains McmA, -B and -C. Analysis of the genome context of MCMs in the latter group indicates that these genes could have arisen from phage-mediated events. When co-expressed in Escherichia coli, the four MCMs from M. maripaludis co-purify, indicating the formation of heteromeric complexes in vitro. The presence of homologues from both groups in all Methanococcales indicates that there could be functionally important differences between these proteins and that Methanococcales MCMs may therefore provide an interesting additional model for eukaryotic MCM function.

摘要

在真核生物中,六个高度相关的微小染色体维持 (MCM) 蛋白复合物被认为是复制解旋酶的功能单位。直到最近,探索真核 MCM 功能的分子机制的系统在生物化学上还难以解决。为了克服这一困难,人们使用古菌的 MCM 同源物进行了 MCM 功能的分子研究。迄今为止,研究过的古菌 MCM 系统只拥有一个功能性 MCM,它形成一个同六聚体复合物,显示出 DNA 结合、ATP 酶和解旋酶活性。我们已经确定了一个具有多个 MCM 同源物的古菌目。对现有的 Methanococcales 基因组的blast 搜索显示,该目成员拥有 2 到 8 个 MCM 同源物。系统发育分析表明,Methanococcales 中的一次古老复制产生了两组主要的 MCM。一组包含 Methanococcus maripaludis S2 McmD,具有与真核 MCM3 中观察到的保守 C 端插入相似的插入,而另一组包含 McmA、-B 和 -C。对后者组中 MCM 基因的基因组环境分析表明,这些基因可能是由噬菌体介导的事件产生的。当在大肠杆菌中共同表达时,M. maripaludis 的四个 MCM 可以共同纯化,表明在体外形成异源六聚体复合物。所有 Methanococcales 都存在这两组同源物,表明这些蛋白之间可能存在功能上的重要差异,并且 Methanococcales MCM 可能因此为真核 MCM 功能提供了一个有趣的额外模型。

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