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RrgA 和 RrgC 通过 C-2 和 C-3 分类酶在肺炎链球菌菌毛中的关联。

Association of RrgA and RrgC into the Streptococcus pneumoniae pilus by sortases C-2 and C-3.

机构信息

Institut de Biologie Structurale Jean-Pierre Ebel, Grenoble, France.

出版信息

Biochemistry. 2012 Jan 10;51(1):342-52. doi: 10.1021/bi201591n. Epub 2011 Dec 7.

DOI:10.1021/bi201591n
PMID:22122269
Abstract

Pili are surface-exposed virulence factors involved in the adhesion of bacteria to host cells. The human pathogen Streptococcus pneumoniae expresses a pilus composed of three structural proteins, RrgA, RrgB, and RrgC, and requires the action of three transpeptidase enzymes, sortases SrtC-1, SrtC-2, and SrtC-3, to covalently associate the Rrg pilins. Using a recombinant protein expression platform, we have previously shown the requirement of SrtC-1 in RrgB fiber formation and the association of RrgB with RrgC. To gain insights into the substrate specificities of the two other sortases, which remain controversial, we have exploited the same robust strategy by testing various combinations of pilins and sortases coexpressed in Escherichia coli. We demonstrate that SrtC-2 catalyzes the formation of both RrgA-RrgB and RrgB-RrgC complexes. The deletion and swapping of the RrgA-YPRTG and RrgB-IPQTG sorting motifs indicate that SrtC-2 preferentially recognizes RrgA and attaches it to the pilin motif lysine 183 of RrgB. Finally, SrtC-2 is also able to catalyze the multimerization of RrgA through the C-terminal D4 domains. Similar experiments have been performed with SrtC-3, which catalyzes the formation of RrgB-RrgC and RrgB-RrgA complexes. Altogether, these results provide evidence of the molecular mechanisms of association of RrgA and RrgC with the RrgB fiber shaft by SrtC-2 and SrtC-3 and lead to a revised model of the pneumococcal pilus architecture accounting for the respective contribution of each sortase.

摘要

菌毛是细菌黏附宿主细胞的表面毒力因子。人类病原体肺炎链球菌表达一种由三种结构蛋白 RrgA、RrgB 和 RrgC 组成的菌毛,需要三种转肽酶酶 SrtC-1、SrtC-2 和 SrtC-3 的作用,才能将 Rrg 菌毛共价偶联。使用重组蛋白表达平台,我们之前已经证明了 SrtC-1 在 RrgB 纤维形成和 RrgB 与 RrgC 结合中的作用。为了深入了解另外两种转肽酶 SrtC-2 和 SrtC-3 的底物特异性,我们利用相同的强大策略,测试了大肠杆菌中各种组合的菌毛和转肽酶的共表达,以获得对这两种转肽酶的深入了解。我们证明了 SrtC-2 催化 RrgA-RrgB 和 RrgB-RrgC 复合物的形成。RrgA-YPRTG 和 RrgB-IPQTG 排序基序的缺失和交换表明,SrtC-2 优先识别 RrgA,并将其附着在 RrgB 的 pilin 基序赖氨酸 183 上。最后,SrtC-2 还能够通过 C 端 D4 结构域催化 RrgA 的多聚化。用 SrtC-3 进行了类似的实验,SrtC-3 催化 RrgB-RrgC 和 RrgB-RrgA 复合物的形成。总之,这些结果为 SrtC-2 和 SrtC-3 将 RrgA 和 RrgC 与 RrgB 纤维轴偶联的分子机制提供了证据,并导致了肺炎球菌菌毛结构的修订模型,该模型考虑了每种转肽酶的各自贡献。

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