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肺炎链球菌中sortase介导的菌毛纤维生物合成

Sortase-mediated pilus fiber biogenesis in Streptococcus pneumoniae.

作者信息

Manzano Clothilde, Contreras-Martel Carlos, El Mortaji Lamya, Izoré Thierry, Fenel Daphna, Vernet Thierry, Schoehn Guy, Di Guilmi Anne Marie, Dessen Andréa

机构信息

Laboratoire des Protéines Membranaires, Institut de Biologie Structurale Jean-Pierre Ebel, UMR 5075 (CEA, CNRS, UJF, PSB), 41 rue Jules Horowitz, F-38027 Grenoble, France.

出版信息

Structure. 2008 Dec 10;16(12):1838-48. doi: 10.1016/j.str.2008.10.007.

Abstract

Streptococcus pneumoniae is a piliated pathogen whose ability to circumvent vaccination and antibiotic treatment strategies is a cause of mortality worldwide. Pili play important roles in pneumococcal infection, but little is known about their biogenesis mechanism or the relationship between components of the pilus-forming machinery, which includes the fiber pilin (RrgB), two minor pilins (RrgA, RrgC), and three sortases (SrtC-1, SrtC-2, SrtC-3). Here we show that SrtC-1 is the main pilus-polymerizing transpeptidase, and electron microscopy analyses of RrgB fibers reconstituted in vitro reveal that they structurally mimic the pneumococcal pilus backbone. Crystal structures of both SrtC-1 and SrtC-3 reveal active sites whose access is controlled by flexible lids, unlike in non-pilus sortases, and suggest that substrate specificity is dictated by surface recognition coupled to lid opening. The distinct structural features of pilus-forming sortases suggest a common pilus biogenesis mechanism that could be exploited for the development of broad-spectrum antibacterials.

摘要

肺炎链球菌是一种有菌毛的病原体,其规避疫苗接种和抗生素治疗策略的能力是全球范围内导致死亡的一个原因。菌毛在肺炎球菌感染中发挥着重要作用,但对于其生物合成机制或菌毛形成机制各组分之间的关系却知之甚少,菌毛形成机制包括纤维菌毛蛋白(RrgB)、两种次要菌毛蛋白(RrgA、RrgC)以及三种分选酶(SrtC-1、SrtC-2、SrtC-3)。在此我们表明,SrtC-1是主要的菌毛聚合转肽酶,对体外重组的RrgB纤维进行的电子显微镜分析显示,它们在结构上模拟了肺炎球菌菌毛主干。SrtC-1和SrtC-3的晶体结构均揭示了其活性位点,与非菌毛分选酶不同,这些活性位点的可及性由柔性盖子控制,这表明底物特异性是由与盖子打开相关的表面识别所决定的。形成菌毛的分选酶的独特结构特征提示了一种共同的菌毛生物合成机制,可用于开发广谱抗菌药物。

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