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YneA,枯草芽孢杆菌中 SOS 诱导的细胞分裂抑制剂,受翻译后调控,并且需要跨膜区域发挥活性。

YneA, an SOS-induced inhibitor of cell division in Bacillus subtilis, is regulated posttranslationally and requires the transmembrane region for activity.

机构信息

Department of Biology, Stanford University, 371 Serra Mall, Stanford, CA 94305-5020, USA.

出版信息

J Bacteriol. 2010 Jun;192(12):3159-73. doi: 10.1128/JB.00027-10. Epub 2010 Apr 16.

Abstract

Cell viability depends on the stable transmission of genetic information to each successive generation. Therefore, in the event of intrinsic or extrinsic DNA damage, it is important that cell division be delayed until DNA repair has been completed. In Bacillus subtilis, this is accomplished in part by YneA, an inhibitor of division that is induced as part of the SOS response. We sought to gain insight into the mechanism by which YneA blocks cell division and the processes involved in shutting off YneA activity. Our data suggest that YneA is able to inhibit daughter cell separation as well as septum formation. YneA contains a LysM peptidoglycan binding domain and is predicted to be exported. We established that the YneA signal peptide is rapidly cleaved, resulting in secretion of YneA into the medium. Mutations within YneA affect both the rate of signal sequence cleavage and the activity of YneA. YneA does not stably associate with the cell wall and is rapidly degraded by extracellular proteases. Based on these results, we hypothesize that exported YneA is active prior to signal peptide cleavage and that proteolysis contributes to the inactivation of YneA. Finally, we identified mutations in the transmembrane segment of YneA that abolish the ability of YneA to inhibit cell division, while having little or no effect on YneA export or stability. These data suggest that protein-protein interactions mediated by the transmembrane region may be required for YneA activity.

摘要

细胞活力依赖于遗传信息稳定地传递到每一代。因此,在发生内在或外在的 DNA 损伤时,重要的是延迟细胞分裂,直到 DNA 修复完成。在枯草芽孢杆菌中,部分通过 YneA 实现这一点,YneA 是一种抑制分裂的物质,作为 SOS 反应的一部分被诱导。我们试图深入了解 YneA 阻止细胞分裂的机制以及关闭 YneA 活性的过程。我们的数据表明,YneA 能够抑制子细胞分离和隔膜形成。YneA 包含一个 LysM 肽聚糖结合结构域,预计被分泌。我们确定 YneA 的信号肽被快速切割,导致 YneA 分泌到培养基中。YneA 内的突变会影响信号序列切割的速度和 YneA 的活性。YneA 不会与细胞壁稳定结合,而是被细胞外蛋白酶迅速降解。基于这些结果,我们假设分泌的 YneA 在信号肽切割之前具有活性,并且蛋白酶解有助于 YneA 的失活。最后,我们鉴定了 YneA 的跨膜片段中的突变,这些突变使 YneA 失去抑制细胞分裂的能力,而对 YneA 的分泌或稳定性几乎没有影响。这些数据表明,跨膜区域介导的蛋白质-蛋白质相互作用可能是 YneA 活性所必需的。

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