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Crystal structure of π initiator protein–iteron complex of plasmid R6K: Implications for initiation of plasmid DNA replication

机译:质粒R6K的π起始蛋白-铁复合物的晶体结构:质粒DNA复制的起始意义

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摘要

We have determined the crystal structure of a monomeric biologically active form of the π initiator protein of plasmid R6K as a complex with a single copy of its cognate DNA-binding site (iteron) at 3.1-Å resolution. The initiator belongs to the family of winged helix type of proteins. The structure reveals that the protein contacts the iteron DNA at two primary recognition helices, namely the C-terminal α4′ and the N-terminal α4 helices, that recognize the 5′ half and the 3′ half of the 22-bp iteron, respectively. The base-amino acid contacts are all located in α4′, whereas the α4 helix and its vicinity mainly contact the phosphate groups of the iteron. Mutational analyses show that the contacts of both recognition helices with DNA are necessary for iteron binding and replication initiation. Considerations of a large number of site-directed mutations reveal that two distinct regions, namely α2 and α5 and its vicinity, are required for DNA looping and initiator dimerization, respectively. Further analysis of mutant forms of π revealed the possible domain that interacts with the DnaB helicase. Thus, the structure–function analysis presented illuminates aspects of initiation mechanism of R6K and its control.
机译:我们已经确定了质粒R6K的π起始蛋白的单体生物活性形式的晶体结构,该结构具有3.1Å分辨率的单拷贝其同源DNA结合位点(铁)。引发剂属于有翼螺旋型蛋白质家族。该结构揭示了该蛋白在两个主要识别螺旋上分别与iteron DNA接触,即C端α4'和N端α4螺旋,它们分别识别22 bp iteron的5'一半和3'一半。 。碱基-氨基酸接触均位于α4'中,而α4螺旋及其附近主要接触异核的磷酸基。突变分析表明,两个识别螺旋与DNA的接触对于iteron结合和复制起始是必需的。对大量定点突变的考虑表明,DNA环化和引发剂二聚化分别需要两个不同的区域,即α2和α5及其附近。对π突变形式的进一步分析揭示了与DnaB解旋酶相互作用的可能域。因此,提出的结构-功能分析阐明了R6K的引发机理及其控制方面。

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