首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Structures of two core subunits of the bacterial type Ⅳ secretion system, VirB8 from Brucella suis and ComB10 from Helicobacter pylori
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Structures of two core subunits of the bacterial type Ⅳ secretion system, VirB8 from Brucella suis and ComB10 from Helicobacter pylori

机译:细菌Ⅳ型分泌系统的两个核心亚基的结构,来自猪布鲁氏菌的VirB8和来自幽门螺杆菌的ComB10

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Type Ⅳ secretion systems (T4SSs) are commonly used secretion machineries in Gram-negative bacteria. They are used in the infection of human, animal, or plant cells and the propagation of antibiotic resistance. The T4SS apparatus spans both membranes of the bacterium and generally is composed of 12 proteins, named VirB1-11 and VirD4 after proteins of the canonical Agrobacterium tumefaciens T4SS. The periplasmic core complex of VirB8, VirB10 structurally and functionally links the cytoplasmic NTPases of the system with its outer membrane and pilus components. Here we present crystal structures of VirB8 of Brucella suis, the causative agent of brucellosis, and ComB10, a VirB10 homolog of Helicobacter pylori, the causative agent of gastric ulcers. The structures of VirB8 and ComB10 resemble known folds, albeit with novel secondary-structure modifications unique to and conserved within their respective families. Both proteins crystallized as dimers, providing detailed predictions about their self associations. These structures make a substantial contribution to the repertoire of T4SS component structures and will serve as springboards for future functional and protein-protein interaction studies by using knowledge-based site-directed and deletion mutagenesis.
机译:Ⅳ型分泌系统(T4SSs)是革兰氏阴性细菌中常用的分泌机制。它们被用于人类,动物或植物细胞的感染以及抗生素抗性的传播。 T4SS装置跨过细菌的两个膜,通常由12种蛋白质组成,分别是标准农杆菌T4SS的蛋白质,分别称为VirB1-11和VirD4。 VirB8,VirB10的周质核心复合物在结构上和功能上将系统的细胞质NTPase与它的外膜和菌毛成分相连。在这里,我们介绍了布鲁氏菌病的病原体猪布鲁氏菌的VirB8和胃溃疡的病原体幽门螺杆菌的VirB10同源物ComB10的晶体结构。 VirB8和ComB10的结构类似于已知的折叠,尽管具有新颖的二级结构修饰,这些修饰是它们各自家族中唯一的并且在它们各自的家族中都保守。两种蛋白质均结晶为二聚体,提供了有关其自身缔合的详细预测。这些结构为T4SS组件结构库做出了重大贡献,并将通过使用基于知识的定点和缺失诱变作为未来功能和蛋白质-蛋白质相互作用研究的跳板。

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