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首页> 外文期刊>Journal of bacteriology >Identification of Multiple Substrates of the StkP Ser/Thr Protein Kinase in Streptococcus pneumoniae
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Identification of Multiple Substrates of the StkP Ser/Thr Protein Kinase in Streptococcus pneumoniae

机译:肺炎链球菌中StkP Ser / Thr蛋白激酶的多种底物的鉴定

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Monitoring the external environment and responding to its changes are essential for the survival of all living organisms. The transmission of extracellular signals in prokaryotes is mediated mainly by two-component systems. In addition, genomic analyses have revealed that many bacteria contain eukaryotic-type Ser/Thr protein kinases. The human pathogen Streptococcus pneumoniae encodes 13 two-component systems and has a single copy of a eukaryotic-like Ser/Thr protein kinase gene designated stkP. Previous studies demonstrated the pleiotropic role of the transmembrane protein kinase StkP in pneumococcal physiology. StkP regulates virulence, competence, and stress resistance and plays a role in the regulation of gene expression. To determine the intracellular signaling pathways controlled by StkP, we used a proteomic approach for identification of its substrates. We detected six proteins phosphorylated on threonine by StkP continuously during growth. We identified three new substrates of StkP: the Mn-dependent inorganic pyrophosphatase PpaC, the hypothetical protein spr0334, and the cell division protein DivIVA. Contrary to the results of a previous study, we did not confirm that the α-subunit of RNA polymerase is a target of StkP. We showed that StkP activation and substrate recognition depend on the presence of a peptidoglycan-binding domain comprising four extracellular penicillin-binding protein- and Ser/Thr kinase-associated domain (PASTA domain) repeats. We found that StkP is regulated in a growth-dependent manner and likely senses intracellular peptidoglycan subunits present in the cell division septa. In addition, stkP inactivation results in cell division defects. Thus, the data presented here suggest that StkP plays an important role in the regulation of cell division in pneumococcus.
机译:监测外部环境并对其变化做出响应对于所有活生物体的生存至关重要。细胞外信号在原核生物中的传递主要由两组分系统介导。此外,基因组分析表明,许多细菌都含有真核型Ser / Thr蛋白激酶。人类病原体肺炎链球菌编码13个两组分系统,并具有一个单一拷贝的真核样Ser / Thr蛋白激酶基因,称为 stkP 。先前的研究证明跨膜蛋白激酶StkP在肺炎球菌生理中的多效性作用。 StkP调节毒力,能力和抗逆性,并在基因表达的调节中发挥作用。为了确定由StkP控制的细胞内信号传导途径,我们使用了蛋白质组学方法来鉴定其底物。在生长过程中,我们连续检测到六种蛋白质被StkP磷酸化在苏氨酸上。我们确定了StkP的三个新的底物:锰依赖性无机焦磷酸酶PpaC,假设的蛋白spr0334和细胞分裂蛋白DivIVA。与先前的研究结果相反,我们没有证实RNA聚合酶的α亚基是StkP的靶标。我们显示StkP激活和底物识别取决于肽聚糖结合结构域的存在,该结构域包含四个细胞外青霉素结合蛋白和Ser / Thr激酶相关结构域(PASTA结构域)重复。我们发现StkP以增长依赖的方式受到监管,并有可能感觉到细胞分裂间隔中存在的细胞内肽聚糖亚基。此外, stkP 失活会导致细胞分裂缺陷。因此,此处提供的数据表明StkP在肺炎球菌的细胞分裂调节中起重要作用。

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