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P1 ParA在parS位点与P1分区复合体相互作用,并且一个ATP-ADP开关控制着ParA的活性。

P1 ParA interacts with the P1 partition complex at parS and an ATP-ADP switch controls ParA activities.

作者信息

Bouet J Y, Funnell B E

机构信息

Department of Molecular and Medical Genetics, University of Toronto, Toronto, Ontario, M5S 1A8, Canada.

出版信息

EMBO J. 1999 Mar 1;18(5):1415-24. doi: 10.1093/emboj/18.5.1415.

Abstract

The partition system of P1 plasmids is composed of two proteins, ParA and ParB, and a cis-acting site parS. parS is wrapped around ParB and Escherichia coli IHF protein in a higher order nucleoprotein complex called the partition complex. ParA is an ATPase that autoregulates the expression of the par operon and has an essential but unknown function in the partition process. In this study we demonstrate a direct interaction between ParA and the P1 partition complex. The interaction was strictly dependent on ParB and ATP. The consequence of this interaction depended on the ParB concentration. At high ParB levels, ParA was recruited to the partition complex via a ParA-ParB interaction, but at low ParB levels, ParA removed or disassembled ParB from the partition complex. ADP could not support these interactions, but could promote the site-specific DNA binding activity of ParA to parOP, the operator of the par operon. Conversely, ATP could not support a stable interaction of ParA with parOP in this assay. Our data suggest that ParA-ADP is the repressor of the par operon, and ParA-ATP, by interacting with the partition complex, plays a direct role in partition. Therefore, one role of adenine nucleotide binding and hydrolysis by ParA is that of a molecular switch controlling entry into two separate pathways in which ParA plays different roles.

摘要

P1质粒的分配系统由两种蛋白质ParA和ParB以及一个顺式作用位点parS组成。parS在一种称为分配复合物的高阶核蛋白复合物中与ParB和大肠杆菌整合宿主因子(IHF)蛋白缠绕在一起。ParA是一种ATP酶,可自动调节par操纵子的表达,并且在分配过程中具有重要但未知的功能。在本研究中,我们证明了ParA与P1分配复合物之间存在直接相互作用。这种相互作用严格依赖于ParB和ATP。这种相互作用的结果取决于ParB的浓度。在高ParB水平下,ParA通过ParA-ParB相互作用被招募到分配复合物中,但在低ParB水平下,ParA从分配复合物中去除或拆解ParB。ADP不能支持这些相互作用,但可以促进ParA与par操纵子的操纵基因parOP的位点特异性DNA结合活性。相反,在该实验中ATP不能支持ParA与parOP的稳定相互作用。我们的数据表明,ParA-ADP是par操纵子的阻遏物,而ParA-ATP通过与分配复合物相互作用,在分配过程中发挥直接作用。因此,ParA结合和水解腺嘌呤核苷酸的一个作用是作为一个分子开关,控制进入ParA发挥不同作用的两条独立途径。

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