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功能性重组脑膜炎球菌转铁蛋白结合蛋白A的表达与纯化

Expression and purification of functional recombinant meningococcal transferrin-binding protein A.

作者信息

Oakhill Jonathan S, Joannou Christopher L, Buchanan Susan K, Gorringe Andrew R, Evans Robert W

机构信息

Metalloprotein Research Group, The Randall Centre for Molecular Mechanisms of Cell Function, King's College London, London SE1 1UL, UK.

出版信息

Biochem J. 2002 Jun 15;364(Pt 3):613-6. doi: 10.1042/BJ20020500.

Abstract

Pathogenic bacteria of the genus Neisseria have a siderophore-independent iron-uptake system reliant on a direct interaction between the bacterial cell and human transferrin (hTf), a serum protein. In the meningococcus, this uptake system is dependent on two surface-exposed, transferrin-binding proteins (Tbps), TbpA and TbpB. TbpA is highly conserved among meningococcal strains, and is thought to be a porin-like integral protein that functions as a gated channel for the passage of iron into the periplasm. TbpB is more variable in size, lipidated and fully surface-exposed. Given its location on the cell surface, its role in pathogenicity and interstrain sequence conservation, TbpA is currently being regarded for inclusion in a meningococcal vaccine effective against all serogroups. This requires gaining knowledge of the ligand-receptor interactions. In the present study we have optimized a procedure for obtaining purified, functionally active recombinant TbpA at a level and stability necessary for the initiation of such studies.

摘要

奈瑟菌属的致病细菌有一种不依赖铁载体的铁摄取系统,该系统依赖于细菌细胞与血清蛋白人转铁蛋白(hTf)之间的直接相互作用。在脑膜炎奈瑟菌中,这种摄取系统依赖于两种表面暴露的转铁蛋白结合蛋白(Tbps),即TbpA和TbpB。TbpA在脑膜炎奈瑟菌菌株中高度保守,被认为是一种类似孔蛋白的整合蛋白,作为铁进入周质的门控通道发挥作用。TbpB的大小更具变异性,有脂质化且完全暴露于表面。鉴于其在细胞表面的位置、在致病性中的作用以及菌株间序列保守性,TbpA目前被考虑纳入一种对所有血清群均有效的脑膜炎奈瑟菌疫苗中。这需要了解配体 - 受体相互作用。在本研究中,我们优化了一种程序,以获得纯化的、具有功能活性的重组TbpA,其水平和稳定性对于启动此类研究是必要的。

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Iron acquisition systems in the pathogenic Neisseria.致病性奈瑟菌中的铁获取系统。
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