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遗传重组中的同源配对:RecA蛋白使缺口环状DNA和闭环状DNA形成联合分子。

Homologous pairing in genetic recombination: recA protein makes joint molecules of gapped circular DNA and closed circular DNA.

作者信息

Cunningham R P, DasGupta C, Shibata T, Radding C M

出版信息

Cell. 1980 May;20(1):223-35. doi: 10.1016/0092-8674(80)90250-0.

Abstract

The recA protein, which is essential for genetic recombination in E. coli, promotes the homologous pairing of double-stranded DNA and linear single-stranded DNA, thereby forming a three-stranded joint molecule called a D loop. Single-stranded DNA stimulates recA protein to unwind double-stranded DNA. By a presumably related mechanism, recA protein promoted the homologous pairing of two circular double-stranded molecules when one of them has a gap in one strand. The two molecules were joined at homologous sites by noncovalent bonds. The covalently closed molecule remained intact and was not topologically linked to the intact circular strand of the gapped substrate. Electron microscopy showed that molecules were usually linked at two or more nearby points. The junctions in most molecules were shorter than 300 nucleotides. Sometimes the region between two extreme points was separated into two arms, producing an ellipsoidal loop (called an eye loop). The junctions in these biparental joint molecules were frequently remote from the site of the gap. We infer that a free end of the interrupted strand crosseover to form a structure like a D loop which moved away from the gap by branch migration.

摘要

RecA蛋白对大肠杆菌的基因重组至关重要,它能促进双链DNA与线性单链DNA的同源配对,从而形成一种称为D环的三链连接分子。单链DNA刺激RecA蛋白解开双链DNA。通过一种可能相关的机制,当其中一个环状双链分子的一条链上有缺口时,RecA蛋白促进两个环状双链分子的同源配对。这两个分子通过非共价键在同源位点连接。共价闭合的分子保持完整,并且在拓扑结构上不与有缺口底物的完整环状链相连。电子显微镜显示分子通常在两个或更多相邻点连接。大多数分子中的连接点短于300个核苷酸。有时两个端点之间的区域会分成两个臂,形成一个椭圆形环(称为眼环)。这些双亲连接分子中的连接点常常远离缺口位点。我们推断,中断链的一个自由端交叉形成一个类似D环的结构,该结构通过分支迁移远离缺口。

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