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质粒分配与P1分配蛋白ParB的扩散

Plasmid partitioning and the spreading of P1 partition protein ParB.

作者信息

Rodionov Oleg, Yarmolinsky Michael

机构信息

Laboratory of Biochemistry, National Cancer Institute, NIH, Bldg 37, Room 6044C, 37 Convent Drive, Bethesda, MD 20892-4255, USA.

出版信息

Mol Microbiol. 2004 May;52(4):1215-23. doi: 10.1111/j.1365-2958.2004.04055.x.

Abstract

Bacterial plasmids of low copy number, P1 prophage among them, are actively partitioned to nascent daughter cells. The process is typically mediated by a pair of plasmid-encoded proteins and a cis-acting DNA site or cluster of sites, referred to as the plasmid centromere. P1 ParB protein, which binds to the P1 centromere (parS), can spread for several kilobases along flanking DNA. We argue that studies of mutant ParB that demonstrated a strong correlation between spreading capacity and the ability to engage in partitioning may be misleading, and describe here a critical test of the dependence of partitioning on the spreading of the wild-type protein. Physical constraints imposed on the spreading of P1 ParB were found to have only a minor, but reproducible, effect on partitioning. We conclude that, whereas extensive ParB spreading is not required for partitioning, spreading may have an auxiliary role in the process.

摘要

低拷贝数的细菌质粒,包括其中的P1原噬菌体,会被主动分配到新生的子细胞中。这个过程通常由一对质粒编码的蛋白质和顺式作用DNA位点或位点簇介导,这些位点被称为质粒着丝粒。与P1着丝粒(parS)结合的P1 ParB蛋白,可以沿着侧翼DNA延伸数千个碱基对。我们认为,对突变型ParB的研究表明,其扩散能力与参与分配的能力之间存在很强的相关性,这可能会产生误导,并在此描述了对野生型蛋白分配依赖于扩散的关键测试。发现施加在P1 ParB扩散上的物理限制对分配只有轻微但可重复的影响。我们得出结论,虽然广泛的ParB扩散不是分配所必需的,但扩散可能在这个过程中起到辅助作用。

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