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UvrD2 在结核分枝杆菌中是必需的,但它的解旋酶活性不是必需的。

UvrD2 is essential in Mycobacterium tuberculosis, but its helicase activity is not required.

机构信息

MRC National Institute for Medical Research, The Ridgeway, Mill Hill, London NW7 1AA, UK.

出版信息

J Bacteriol. 2011 Sep;193(17):4487-94. doi: 10.1128/JB.00302-11. Epub 2011 Jul 1.

Abstract

UvrD is an SF1 family helicase involved in DNA repair that is widely conserved in bacteria. Mycobacterium tuberculosis has two annotated UvrD homologues; here we investigate the role of UvrD2. The uvrD2 gene at its native locus could be knocked out only in the presence of a second copy of the gene, demonstrating that uvrD2 is essential. Analysis of the putative protein domain structure of UvrD2 shows a distinctive domain architecture, with an extended C terminus containing an HRDC domain normally found in SF2 family helicases and a linking domain carrying a tetracysteine motif. Truncated constructs lacking the C-terminal domains of UvrD2 were able to compensate for the loss of the chromosomal copy, showing that these C-terminal domains are not essential. Although UvrD2 is a functional helicase, a mutant form of the protein lacking helicase activity was able to permit deletion of uvrD2 at its native locus. However, a mutant protein unable to hydrolyze ATP or translocate along DNA was not able to compensate for lack of the wild-type protein. Therefore, we concluded that the essential role played by UvrD2 is unlikely to involve its DNA unwinding activity and is more likely to involve DNA translocation and, possibly, protein displacement.

摘要

UvrD 是一种 SF1 家族解旋酶,参与 DNA 修复,在细菌中广泛保守。结核分枝杆菌有两个注释的 UvrD 同源物;在这里,我们研究了 UvrD2 的作用。只有在第二个基因拷贝的存在下,才能在天然基因座敲除 uvrD2 基因,这表明 uvrD2 是必需的。对 UvrD2 的假定蛋白质结构域分析表明,其具有独特的结构域架构,其延伸的 C 末端包含 HRDC 结构域,通常在 SF2 家族解旋酶中发现,以及带有四半胱氨酸基序的连接结构域。缺乏 UvrD2 的 C 末端结构域的截断构建体能够补偿染色体拷贝的缺失,表明这些 C 末端结构域不是必需的。尽管 UvrD2 是一种功能性解旋酶,但缺乏解旋酶活性的蛋白质突变体能够在其天然基因座上允许 uvrD2 的缺失。然而,不能水解 ATP 或沿 DNA 易位的突变体蛋白不能补偿野生型蛋白的缺失。因此,我们得出结论,UvrD2 发挥的必需作用不太可能涉及其 DNA 解旋活性,而更可能涉及 DNA 易位和可能的蛋白质位移。

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