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首页> 外文期刊>Nucleic acids research >Domain mapping of Escherichia coli RecQ defines the roles of conserved N‐ and C‐terminal regions in the RecQ family
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Domain mapping of Escherichia coli RecQ defines the roles of conserved N‐ and C‐terminal regions in the RecQ family

机译:大肠杆菌RecQ的域映射定义了RecQ家族中保守的N和C末端区域的作用

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RecQ DNA helicases function in DNA replication, recombination and repair. Although the precise cellular roles played by this family of enzymes remain elusive, the importance of RecQ proteins is clear; mutations in any of three human RecQ genes lead to genomic instability and cancer. In this report, proteolysis is used to define a two‐domain structure for Escherichia coli RecQ, revealing a large (~59 kDa) N‐terminal and a small (~9 kDa) C‐terminal domain. A short N‐terminal segment (7 or 21 residues) is also shown to be sensitive to proteases. The effects of removing these regions of RecQ are tested in vitro. Removing 21 N‐terminal residues from RecQ severely diminishes its DNA‐dependent ATPase and helicase activities, but does not affect its ability to bind DNA in electrophoretic mobility shift assays. In contrast, removing the ~9 kDa C‐terminal domain from RecQ results in a fragment with normal levels of ATPase and helicase activity, but that has lost the ability to stably associate with DNA. These results establish the biochemical roles of an N‐terminal sequence motif in RecQ catalytic function and for the C‐terminal RecQ domain in stable DNA binding.
机译:RecQ DNA解旋酶在DNA复制,重组和修复中起作用。尽管该酶家族所发挥的确切细胞作用仍然难以捉摸,但RecQ蛋白的重要性却很明显。三个人类RecQ基因中任何一个的突变都会导致基因组不稳定和癌症。在本报告中,蛋白水解用于定义大肠杆菌RecQ的两个结构域结构,揭示了一个大(〜59 kDa)N末端和一个小(〜9 kDa)C末端结构域。短的N末端片段(7或21个残基)也显示对蛋白酶敏感。体外测试去除RecQ这些区域的效果。从RecQ中去除21个N端残基会严重降低其DNA依赖性ATPase和解旋酶的活性,但不会影响其在电泳迁移率迁移分析中与DNA结合的能力。相比之下,从RecQ去除〜9 kDa C末端结构域会产生具有正常水平的ATPase和解旋酶活性的片段,但已经失去了与DNA稳定缔合的能力。这些结果确定了Rec催化功能中N末端序列基序的稳定生化作用以及稳定DNA结合中C末端RecQ结构域的生化作用。

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