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关于大肠杆菌的recA蛋白和单链DNA结合蛋白使单链和双链DNA分子配对的机制

On the mechanism of pairing of single- and double-stranded DNA molecules by the recA and single-stranded DNA-binding proteins of Escherichia coli.

作者信息

Julin D A, Riddles P W, Lehman I R

出版信息

J Biol Chem. 1986 Jan 25;261(3):1025-30.

PMID:3511041
Abstract

The pairing of single- and double-stranded DNA molecules at homologous sequences promoted by recA and single-stranded DNA-binding proteins of Escherichia coli follows apparent first-order kinetics. The initial rate and first-order rate constant for the reaction are maximal at approximately 1 recA protein/3 and 1 single-stranded DNA-binding protein/8 nucleotides of single-stranded DNA. The initial rate increases with the concentration of duplex DNA; however, the rate constant is independent of duplex DNA concentration. Both the rate constant and extent of reaction increase linearly with increasing length of duplex DNA over the range 366 to 8623 base pairs. In contrast, the rate constant is independent of the size of the circular single-stranded DNA between 6,400 and 10,100 nucleotides. No significant effect on reaction rate is observed when a single-stranded DNA is paired with 477 base pairs of homologous duplex DNA joined to increasing lengths of heterologous DNA (627-2,367 base pairs). Similarly, heterologous T7 DNA has no effect on the rate of pairing. These findings support a mechanism in which a recA protein-single-stranded DNA complex interacts with the duplex DNA to produce an intermediate in which the two DNA molecules are aligned at homologous sequences. Conversion of the intermediate to a paranemic joint then occurs in a rate-determining unimolecular process.

摘要

由大肠杆菌的recA和单链DNA结合蛋白促进的单链和双链DNA分子在同源序列处的配对遵循明显的一级动力学。反应的初始速率和一级速率常数在大约每3个核苷酸有1个recA蛋白和每8个单链DNA核苷酸有1个单链DNA结合蛋白时最大。初始速率随双链DNA浓度增加而增加;然而,速率常数与双链DNA浓度无关。在366至8623个碱基对的范围内,速率常数和反应程度均随双链DNA长度增加而线性增加。相比之下,速率常数与6400至10100个核苷酸之间的环状单链DNA大小无关。当单链DNA与连接有不断增加长度的异源DNA(627 - 2367个碱基对)的477个碱基对的同源双链DNA配对时,未观察到对反应速率有显著影响。同样,异源T7 DNA对配对速率也没有影响。这些发现支持了一种机制,即recA蛋白 - 单链DNA复合物与双链DNA相互作用产生一种中间体,其中两个DNA分子在同源序列处对齐。然后中间体转化为平行双链体接头的过程发生在一个速率决定的单分子过程中。

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