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肺炎链球菌甲硫氨酸ABC转运蛋白的底物结合蛋白SP_0149底物特异性的结构见解

Structural insights into the substrate specificity of SP_0149, the substrate-binding protein of a methionine ABC transporter from Streptococcus pneumoniae.

作者信息

Jha Bhavya, Vyas Rajan, Bhushan Jaya, Sehgal Devinder, Biswal Bichitra Kumar

机构信息

Structural and Functional Biology Laboratory, National Institute of Immunology, Aruna Asaf Ali Marg, New Delhi 110 067, India.

Molecular Immunology Laboratory, National Institute of Immunology, Aruna Asaf Ali Marg, New Delhi 110 067, India.

出版信息

Acta Crystallogr F Struct Biol Commun. 2019 Jul 1;75(Pt 7):520-528. doi: 10.1107/S2053230X19009038. Epub 2019 Jul 4.

DOI:10.1107/S2053230X19009038
PMID:31282873
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6613447/
Abstract

Successful pathogenesis is a cumulative effect of the virulence factors of a pathogen and its capability to efficiently utilize the available nutrients from the host. Streptococcus pneumoniae, a Gram-positive opportunistic pathogen, may either reside asymptomatically as a nasopharyngeal commensal inside the human host or cause lethal diseases, including pneumonia, meningitis and sepsis. S. pneumoniae is known to acquire methionine (Met) from its host through a Met importer. Here, the crystal structure of the substrate-binding protein (SBP; SP_0149) of an ABC importer with Met bound is reported at a resolution of 1.95 Å. The three-dimensional structure of SBP shows that it is composed of two distinct domains, each consisting of a mixed β-sheet flanked by helices. The substrate, Met, is bound in the central part of the interface between the two domains. The overall structure of SP_0149 resembles those of SBPs from other reported bacterial Met and Gly-Met dipeptide transporters. However, a detailed analysis of these structures shows notable variations in the amino-acid composition of the substrate-binding pockets of the SP_0149-Met and GmpC-Gly-Met structures. In particular, SP_0149 harbors Thr212 and Tyr114, whereas the corresponding residues in GmpC are Gly and Val. This difference is likely to be the underlying basis for their differential substrate specificity. In summary, the structure of the SP_0149-Met complex provides insights into the transport function of SP_0149 and its interactions with methionine. It opens up avenues for the rational design of inhibitors of SP_0149 through a structure-mediated approach.

摘要

成功的致病过程是病原体毒力因子及其有效利用宿主可用营养物质能力的累积效应。肺炎链球菌是一种革兰氏阳性机会致病菌,它既可以作为人类宿主鼻咽部的共生菌无症状地存在,也可以引发致命疾病,包括肺炎、脑膜炎和败血症。已知肺炎链球菌通过一种甲硫氨酸(Met)转运蛋白从宿主获取甲硫氨酸。在此,报道了一种结合有Met的ABC转运蛋白的底物结合蛋白(SBP;SP_0149)的晶体结构,分辨率为1.95 Å。SBP的三维结构表明它由两个不同的结构域组成,每个结构域都由一个两侧有螺旋的混合β折叠组成。底物Met结合在两个结构域之间界面的中心部分。SP_0149的整体结构类似于其他已报道的细菌Met和甘氨酸 - 甲硫氨酸二肽转运蛋白的SBP。然而,对这些结构的详细分析表明,SP_0149 - Met和GmpC - 甘氨酸 - 甲硫氨酸结构的底物结合口袋的氨基酸组成存在显著差异。特别是,SP_0149含有苏氨酸212和酪氨酸114,而GmpC中的相应残基是甘氨酸和缬氨酸。这种差异可能是它们不同底物特异性的潜在基础。总之,SP_0149 - Met复合物的结构为深入了解SP_0149的转运功能及其与甲硫氨酸的相互作用提供了线索。它为通过结构介导的方法合理设计SP_0149抑制剂开辟了途径。

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