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镍在人类病原体中的混杂输入:细胞外镍结合蛋白的结构、热力学和进化。

Promiscuous nickel import in human pathogens: structure, thermodynamics, and evolution of extracytoplasmic nickel-binding proteins.

机构信息

University Grenoble Alpes, Institut de Biologie Structurale (IBS), 38044 Grenoble, France; CNRS, IBS, 38044 Grenoble, France; CEA, IBS, 38044 Grenoble, France.

Université de Lyon, Université Lyon 1, CNRS, UMR5558, Laboratoire de Biométrie et Biologie Evolutive, 43 Boulevard du 11 Novembre 1918, 69622 Villeurbanne, France.

出版信息

Structure. 2014 Oct 7;22(10):1421-32. doi: 10.1016/j.str.2014.07.012. Epub 2014 Sep 4.

Abstract

In human pathogenic bacteria, nickel is required for the activation of two enzymes, urease and [NiFe]-hydrogenase, necessary for host infection. Acquisition of Ni(II) is mediated by either permeases or ABC-importers, the latter including a subclass that involves an extracytoplasmic nickel-binding protein, Ni-BP. This study reports on the structure of three Ni-BPs from a diversity of human pathogens and on the existence of three new nickel-binding motifs. These are different from that previously described for Escherichia coli Ni-BP NikA, known to bind nickel via a nickelophore, and indicate a variegated ligand selectivity for Ni-BPs. The structures are consistent with ligand affinities measured in solution by calorimetry and challenge the hypothesis of a general requirement of nickelophores for nickel uptake by canonical ABC importers. Phylogenetic analyses showed that Ni-BPs have different evolutionary origins and emerged independently from peptide-binding proteins, possibly explaining the promiscuous behavior of this class of Ni(II) carriers.

摘要

在人类致病菌中,镍对于两种酶——脲酶和[NiFe]-氢化酶的激活是必需的,这两种酶对于宿主感染是必要的。镍(II)的获取是通过渗透酶或 ABC 进口器介导的,后者包括一个涉及细胞外镍结合蛋白 Ni-BP 的亚类。本研究报告了来自多种人类病原体的三种 Ni-BP 的结构,以及三种新的镍结合基序的存在。这些与先前描述的大肠杆菌 Ni-BP NikA 不同,NikA 已知通过镍载体结合镍,并表明 Ni-BP 具有多样化的配体选择性。这些结构与通过量热法在溶液中测量的配体亲和力一致,挑战了镍载体对于典型 ABC 进口器摄取镍的普遍要求的假设。系统发育分析表明,Ni-BP 具有不同的进化起源,并且独立于肽结合蛋白出现,这可能解释了这一类 Ni(II)载体的混杂行为。

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