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Structural basis of replication origin recognition by the DnaA protein

机译:DnaA蛋白识别复制起点的结构基础

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Escherichia coli DnaA binds to 9 bp sequences (DnaA) boxes) in the replication origin, oriC, to form a complex initiating chromosomal DNA replication. In the present study, we determined the crystal structure of its DNA-binding domain (domain IV) complexed with a DnaA box at 2.1 A resolution. DnaA domain IV contains a helix-turn-helix motif for DNA binding. One helix and a loop of the helix-turn-helix motif are inserted into the major groove and 5 bp (3' two-thirds of the DnaA box sequence) are recognized through base-specific hydrogen bonds and van der Waals contacts with the C5-methyl groups of thymines. In the minor groove, Arg399, located in the loop adjacent to the motif, recognizes three more base pairs (5' one-third of the DnaA box sequence) by base-specific hydrogen bonds. DNA bending by ~28°was also observed in the complex. These base-specific interactions explain how DnaA exhibits higher affinity for the strong DnaA boxes (R1, R2 and R4) than the weak DnaA boxes (R3 and M) in the replication origin.
机译:大肠杆菌DnaA与复制起点oriC中的9 bp序列(DnaA)盒结合,形成复杂的染色体DNA复制起始。在本研究中,我们确定了其DNA结合域(域IV)与DnaA盒以2.1 A分辨率复合的晶体结构。 DnaA结构域IV包含用于DNA结合的螺旋-转-螺旋基序。将一个螺旋和一个螺旋-转-螺旋基序的环插入主沟,并通过碱基特异性氢键和范德华与C5的接触识别5 bp(DnaA盒序列的3'的三分之二)胸腺嘧啶的-甲基。在较小的凹槽中,位于邻近基序的环中的Arg399通过碱基特异性氢键识别出另外三个碱基对(DnaA盒序列的5'的三分之一)。在该复合物中还观察到〜28°的DNA弯曲。这些特定于碱基的相互作用解释了DnaA如何在复制源中对强DnaA框(R1,R2和R4)表现出比弱DnaA框(R3和M)更高的亲和力。

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