首页> 美国卫生研究院文献>Nucleic Acids Research >DnaG interacts with a linker region that joins the N- and C-domains of DnaB and induces the formation of 3-fold symmetric rings
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DnaG interacts with a linker region that joins the N- and C-domains of DnaB and induces the formation of 3-fold symmetric rings

机译:DnaG与连接器区域相互作用该连接器区域连接DnaB的N和C域并诱导形成3倍对称环

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摘要

Loading of the replicative ring helicase onto the origin of replication (oriC) is the final outcome of a well coordinated series of events that collectively constitute a primosomal cascade. Once the ring helicase is loaded, it recruits the primase and signals the switch to the polymerization mode. The transient nature of the helicase–primase (DnaB–DnaG) interaction in the Escherichia coli system has hindered our efforts to elucidate its structure and function. Taking advantage of the stable DnaB–DnaG complex in Bacillus stearothermophilus, we have reviewed conflicting mutagenic data from other bacterial systems and shown that DnaG interacts with the flexible linker that connects the N- and C-terminal domains of DnaB. Furthermore, atomic force microscopy (AFM) imaging experiments show that binding of the primase to the helicase induces predominantly a 3-fold symmetric morphology to the hexameric ring. Overall, three DnaG molecules appear to interact with the hexameric ring helicase but a small number of complexes with two and even one DnaG molecule bound to DnaB were also detected. The structural/functional significance of these data is discussed and a speculative structural model for this complex is suggested.
机译:将复制环解旋酶加载到复制起点(oriC)上是一系列协调良好的事件的最终结果,这些事件共同构成了原始染色体的级联反应。加载环解酶后,它会募集引发酶并发出切换至聚合模式的信号。大肠杆菌系统中解旋酶-引发酶(DnaB-DnaG)相互作用的瞬时性质阻碍了我们阐明其结构和功能的努力。利用嗜热脂肪芽孢杆菌中稳定的DnaB–DnaG复合物的优势,我们综述了来自其他细菌系统的相互矛盾的诱变数据,并显示了DnaG与连接DnaB N和C末端结构域的柔性接头相互作用。此外,原子力显微镜(AFM)成像实验表明,引发酶与解旋酶的结合主要诱导六聚环的3倍对称形态。总体而言,三个DnaG分子似乎与六聚环解旋酶发生相互作用,但是还检测到少量与两个甚至一个DnaG分子结合到DnaB的复合物。讨论了这些数据的结构/功能意义,并提出了针对该复合物的推测结构模型。

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