必需WalK组氨酸激酶和WalR调节因子差异介导金黄色葡萄球菌RN4220的自溶。

Journal of nature and science Pub Date : 2015-06-01
Li Zheng, Meiying Yan, Frank Fan, Yinduo Ji
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引用次数: 0

摘要

双组分调控系统,WalR/WalK是不同革兰氏阳性细菌生长所必需的,包括金黄色葡萄球菌。本研究以金黄色葡萄球菌RN4220菌株为研究对象,证实了组氨酸激酶蛋白WalK和反应调节因子WalR对葡萄球菌生长的重要性,并证明组氨酸激酶蛋白WalK和反应调节因子WalR在葡萄球菌自溶中的调节作用不同。下调walR表达可有效抑制Triton x -100诱导的细胞裂解,对细菌对青霉素诱导的细胞裂解的耐受性影响较弱。相比之下,walK表达下调对Triton X-100或青霉素引起的自溶均无影响。此外,我们通过酶谱分析确定了WalR和WalK对细菌水解酶活性的影响。结果表明,下调walR表达突变体的细胞裂解液出现细胞壁水解活性降低的条带;然而,WalK的下调对水解活性没有显著影响。进一步,我们检测了WalR对与葡萄球菌自溶相关的cidA转录的影响,结果表明,WalR的下调导致生长对数期cidA转录减少。综上所述,上述结果表明,必需的WalR反应调节因子和必需的WalK组氨酸激酶可能在RN4220菌株中不同程度地控制细菌裂解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

The Essential WalK Histidine Kinase and WalR Regulator Differentially Mediate Autolysis of <i>Staphylococcus aureus</i> RN4220.

The Essential WalK Histidine Kinase and WalR Regulator Differentially Mediate Autolysis of <i>Staphylococcus aureus</i> RN4220.

The Essential WalK Histidine Kinase and WalR Regulator Differentially Mediate Autolysis of <i>Staphylococcus aureus</i> RN4220.

The Essential WalK Histidine Kinase and WalR Regulator Differentially Mediate Autolysis of Staphylococcus aureus RN4220.

The two-component regulatory system, WalR/WalK is necessary for growth of different gram-positive bacteria, including Staphylococcus aureus. In present study, we confirmed the essentiality of both the histidine kinase protein WalK and the response regulator WalR for growth using S. aureus RN4220 strain and demonstrated that the histidine kinase protein WalK and the response regulator WalR function differently in regulation of staphylococcal autolysis. The down-regulation of walR expression effectively inhibited Triton X-100-induced lysis and had a weak impact on bacterial tolerance to penicillin induced cell lysis. In contrast, the down-regulation of walK expression had no influence on either Triton X-100- or penicillin-caused autolysis. Moreover, we determined the effect of WalR and WalK on bacterial hydrolase activity using a zymogram analysis. The results showed that the cell lysate of down-regulated walR expression mutant displayed several bands of decreased cell wall hydrolytic activities; however, the down-regulation of WalK had no dramatic impact on the hydrolytic activities. Furthermore, we examined the impact of WalR on the transcription of cidA associated with staphylococcal autolysis, and the results showed that the down-regulation of WalR led to decreased transcription of cidA in the log phase of growth. Taken together, the above results suggest that the essential WalR response regulator and the essential WalK histidine kinase might differently control bacterial lysis in RN4220 strain.

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