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SprA 丝氨酸整合酶的极端 C 末端元件是控制重组及其方向性的“分子拨动开关”的潜在组成部分。

Extreme C-terminal element of SprA serine integrase is a potential component of the "molecular toggle switch" which controls the recombination and its directionality.

机构信息

Research Center of Micro-Nano Technology, Hosei University, Koganei, Japan.

Department of Frontier Bioscience, Hosei University, Koganei, Japan.

出版信息

Mol Microbiol. 2021 Jun;115(6):1110-1121. doi: 10.1111/mmi.14654. Epub 2020 Dec 13.

Abstract

In Bacillus subtilis, a sporulation-related gene, spsM, is disrupted by SPβ prophage, but reconstituted during sporulation through SPβ excision. The spsM reconstitution is catalyzed by a site-specific DNA recombinase, SprA, and its cognate recombination directionality factor, SprB. SprB interacts with SprA, directing the SprA-mediated recombination reaction from integration to excision; however, the details of the directionality control remains unclear. Here, we demonstrate the importance of the extreme C-terminal region (ECT) of SprA in the DNA recombination and directionality control. We created a series of SprA C-terminal deletants and examined their DNA-binding and recombination activities. Deletions in the ECT caused a loss of integration and excision activity, the magnitudes of which positively correlated with the deletion size. Gel shift study revealed that the loss of the integration activity was attributable to the failure of synaptic complex formation. The excision deficiency was caused by defective interaction with SprB. Moreover, alanine scanning analysis revealed that Phe532 is essential to interact with SprB. SprA , therefore, showed almost no excision activity, while retaining the integration activity. Collectively, these results suggest that the ECT plays the crucial roles in the interaction of SprA with SprB and possibly in the directional control of the recombination.

摘要

在枯草芽孢杆菌中,一个与孢子形成相关的基因 spsM 被 SPβ 噬菌体破坏,但在孢子形成过程中通过 SPβ 切除而重建。spsM 的重建由一个位点特异性 DNA 重组酶 SprA 及其同源重组方向性因子 SprB 催化。SprB 与 SprA 相互作用,指导 SprA 介导的从整合到切除的重组反应;然而,方向控制的细节仍不清楚。在这里,我们证明了 SprA 的极端 C 末端区域(ECT)在 DNA 重组和方向性控制中的重要性。我们创建了一系列 SprA C 末端缺失体,并检查了它们的 DNA 结合和重组活性。ECT 的缺失导致整合和切除活性的丧失,其丧失的程度与缺失的大小呈正相关。凝胶迁移研究表明,整合活性的丧失归因于突触复合物形成的失败。切除缺陷是由于与 SprB 的相互作用缺陷引起的。此外,丙氨酸扫描分析表明,苯丙氨酸 532 对于与 SprB 相互作用是必不可少的。因此,SprA 几乎没有切除活性,而保留了整合活性。总之,这些结果表明 ECT 在 SprA 与 SprB 的相互作用以及重组的定向控制中起着至关重要的作用。

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