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着丝粒分散在稳定线性细菌质粒中的作用。

On the role of centromere dispersion in stability of linear bacterial plasmids.

机构信息

Centre Bioengineering, Russian Academy of Sciences, Moscow 117312, Russia.

出版信息

Plasmid. 2010 Jul;64(1):51-9. doi: 10.1016/j.plasmid.2010.04.001. Epub 2010 Apr 18.

Abstract

The N15 prophage-plasmid is linear, and the four centromere sites that enable its active partition are scattered rather than confined to a tandem array. This unusual arrangement suggested that the two features might be linked: centromere dispersion could enable condensation of linear DNA through interaction of partition complexes and so facilitate movement of segregating plasmid molecules. The present study examines this possibility. Linear N15 derivatives varying in centromere-site (IR) position, number and spacing were constructed, and stabilization of these plasmids by N15 SopAB proteins was measured. Stabilization increased in proportion to the number of IR sites and the distance between IR sites, the result expected if condensation mediated by partition complexes (SopB-IR) improves efficiency of SopA-directed segregation. However, visualization of two IR sites on the same molecule revealed that their colocalization did not depend on SopB but resulted from spontaneous folding of the linear DNA. Segregation of these sites by SopA was limited and incomplete compared to partition of plasmid copies. These observations imply that forces responsible for intrinsic folding of linear DNA tend to counter attempts to partition centromeres in cis to each other. We suggest that the beneficial effects of IR number and spacing on partition stem not from condensation but from provision of more numerous and better arranged substrates for SopA action.

摘要

N15 噬菌体-质粒是线性的,使它能够进行主动分配的四个着丝粒位点分散而不是局限于串联排列。这种不寻常的排列表明这两个特征可能相关:着丝粒的分散可以通过分配复合物的相互作用使线性 DNA 浓缩,从而促进分离质粒分子的运动。本研究检验了这种可能性。构建了着丝粒位点(IR)位置、数量和间隔不同的线性 N15 衍生物,并测量了 N15 SopAB 蛋白对这些质粒的稳定作用。稳定度与 IR 位点的数量和 IR 位点之间的距离成正比,如果由分配复合物(SopB-IR)介导的浓缩提高 SopA 定向分离的效率,则会出现这种结果。然而,对同一分子上的两个 IR 位点的可视化显示,它们的共定位不依赖于 SopB,而是由于线性 DNA 的自发折叠所致。与质粒拷贝的分配相比,SopA 对这些位点的分离是有限和不完全的。这些观察结果表明,负责线性 DNA 内在折叠的力往往会阻碍顺式彼此分配着丝粒的尝试。我们认为,IR 数量和间隔对分配的有益影响不是来自于浓缩,而是来自于为 SopA 作用提供更多数量和更好排列的底物。

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