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真菌病原体获取血红素铁的结构基础。

Structural basis of haem-iron acquisition by fungal pathogens.

机构信息

B. Rappaport Faculty of Medicine, Technion - Israel Institute of Technology, and the Rappaport Institute for Research in the Medical Sciences, Haifa 31096, Israel.

Wolfson Centre for Applied Structural Biology, Hebrew University of Jerusalem, Jerusalem, Israel.

出版信息

Nat Microbiol. 2016 Sep 12;1(11):16156. doi: 10.1038/nmicrobiol.2016.156.

Abstract

Pathogenic microorganisms must cope with extremely low free-iron concentrations in the host's tissues. Some fungal pathogens rely on secreted haemophores that belong to the Common in Fungal Extracellular Membrane (CFEM) protein family, to extract haem from haemoglobin and to transfer it to the cell's interior, where it can serve as a source of iron. Here we report the first three-dimensional structure of a CFEM protein, the haemophore Csa2 secreted by Candida albicans. The CFEM domain adopts a novel helical-basket fold that consists of six α-helices, and is uniquely stabilized by four disulfide bonds formed by its eight signature cysteines. The planar haem molecule is bound between a flat hydrophobic platform located on top of the helical basket and a peripheral N-terminal 'handle' extension. Exceptionally, an aspartic residue serves as the CFEM axial ligand, and so confers coordination of Fe haem, but not of Fe haem. Histidine substitution mutants of this conserved Asp acquired Fe haem binding and retained the capacity to extract haem from haemoglobin. However, His-substituted CFEM proteins were not functional in vivo and showed disturbed haem exchange in vitro, which suggests a role for the oxidation-state-specific Asp coordination in haem acquisition by CFEM proteins.

摘要

病原微生物必须应对宿主组织中极低的游离铁浓度。一些真菌病原体依赖于分泌的属于真菌细胞外膜(CFEM)蛋白家族的血红素载体,从血红蛋白中提取血红素并将其转移到细胞内部,在那里它可以作为铁的来源。在这里,我们报告了第一个 CFEM 蛋白的三维结构,即白色念珠菌分泌的血红素载体 Csa2。CFEM 结构域采用一种新颖的螺旋篮状折叠,由六个α-螺旋组成,由其八个特征半胱氨酸形成的四个二硫键独特地稳定。平面血红素分子被绑定在螺旋篮的顶部的一个平坦的疏水性平台和一个外围的 N 端“手柄”延伸之间。异常的是,天冬氨酸残基作为 CFEM 的轴向配体,因此赋予了 Fe 血红素的配位,但不是 Fe 血红素的配位。这个保守的天冬氨酸残基的组氨酸取代突变体获得了 Fe 血红素的结合能力,并保留了从血红蛋白中提取血红素的能力。然而,His 取代的 CFEM 蛋白在体内没有功能,并且在体外表现出血红素交换紊乱,这表明 CFEM 蛋白在血红素获取中氧化态特异性 Asp 配位的作用。

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