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首页> 外文期刊>Journal of Molecular Biology >ATP binding, ATP hydrolysis, and protein dimerization are required for RecF to catalyze an early step in the processing and recovery of replication forks disrupted by DNA damage.
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ATP binding, ATP hydrolysis, and protein dimerization are required for RecF to catalyze an early step in the processing and recovery of replication forks disrupted by DNA damage.

机译:RecF需要ATP结合,ATP水解和蛋白质二聚化才能催化DNA破坏破坏的复制叉的加工和回收的早期步骤。

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摘要

In Escherichia coli, the recovery of replication following disruption by UV-induced DNA damage requires the RecF protein and occurs through a process that involves stabilization of replication fork DNA, resection of nascent DNA to allow the offending lesion to be repaired, and reestablishment of a productive replisome on the DNA. RecF forms a homodimer and contains an ATP binding cassette ATPase domain that is conserved among eukaryotic SMC (structural maintenance of chromosome) proteins, including cohesin, condensin, and Rad50. Here, we investigated the functions of RecF dimerization, ATP binding, and ATP hydrolysis in the progressive steps involved in recovering DNA synthesis following disruption by DNA damage. RecF point mutations with altered biochemical properties were constructed in the chromosome. We observed that protein dimerization, ATP binding, and ATP hydrolysis were essential for maintaining and processing the arrested replication fork, as well as for restoring DNA synthesis. In contrast, stabilization of the RecF protein dimer partially protected the DNA at the arrested fork from degradation, although overall processing and recovery remained severely impaired.
机译:在大肠杆菌中,受紫外线诱导的DNA破坏破坏后,复制的恢复需要RecF蛋白,并且该过程涉及复制叉DNA的稳定化,新生DNA的切除以使有问题的病变得以修复并重新建立。 DNA上的高效复制体。 RecF形成同源二聚体,并包含一个ATP结合盒ATPase结构域,该结构域在真核SMC(染色体的结构维持)蛋白(包括黏附素,凝缩蛋白和Rad50)之间保守。在这里,我们研究了RecF二聚化,ATP结合和ATP水解的功能,这些过程涉及DNA破坏破坏后恢复DNA合成的过程。在染色体上构建了具有改变的生化特性的RecF点突变。我们观察到蛋白质二聚化,ATP结合和ATP水解对于维持和处理被阻止的复制叉以及恢复DNA合成至关重要。相反,RecF蛋白二聚体的稳定部分保护了被捕叉处的DNA免受降解,尽管总体加工和恢复仍然受到严重损害。

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