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人类Rad51蛋白在体外促进ATP依赖的同源配对和链转移反应。

Human Rad51 protein promotes ATP-dependent homologous pairing and strand transfer reactions in vitro.

作者信息

Baumann P, Benson F E, West S C

机构信息

Imperial Cancer Research Fund, South Mimms, Herts, United Kingdom.

出版信息

Cell. 1996 Nov 15;87(4):757-66. doi: 10.1016/s0092-8674(00)81394-x.

Abstract

The human testis Rad51 protein, a structural homolog of E. coli RecA, binds single- and double-stranded DNA and exhibits DNA-dependent ATPase activity. Using circular ssDNA and linear dsDNA (3.0 kb in length), we demonstrate that hRad51 promotes homologous pairing and strand exchange reactions in vitro. Joint molecule formation was dependent upon ATP hydrolysis and DNA homology and was stimulated by the single-strand DNA-binding protein RP-A. In these reactions, the 5' terminus of the complementary strand of the linear duplex was efficiently transferred to the ssDNA. However, under standard conditions, extensive strand exchange was not observed. These results establish hRad51 as a functional homolog of RecA, but indicate that the human protein and its bacterial counterpart differ in their ability to promote extensive strand transfer. It is proposed that hRad51 mediates homology recognition and initiates strand exchange, but that extensive heteroduplex formation in higher organisms requires the actions of additional proteins.

摘要

人类睾丸Rad51蛋白是大肠杆菌RecA的结构同源物,可结合单链和双链DNA,并具有依赖于DNA的ATP酶活性。利用环状单链DNA和线性双链DNA(长度为3.0 kb),我们证明hRad51在体外促进同源配对和链交换反应。联合分子的形成依赖于ATP水解和DNA同源性,并受到单链DNA结合蛋白RP-A的刺激。在这些反应中,线性双链互补链的5'末端有效地转移到了单链DNA上。然而,在标准条件下,未观察到广泛的链交换。这些结果确立了hRad51作为RecA的功能同源物,但表明人类蛋白质与其细菌对应物在促进广泛链转移的能力上有所不同。有人提出,hRad51介导同源性识别并启动链交换,但高等生物中广泛的异源双链体形成需要其他蛋白质的作用。

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