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白细胞毒素S组分的晶体结构:对葡萄球菌β桶状成孔毒素的新认识

Crystal structure of leucotoxin S component: new insight into the Staphylococcal beta-barrel pore-forming toxins.

作者信息

Guillet Valérie, Roblin Pierre, Werner Sandra, Coraiola Manuela, Menestrina Gianfranco, Monteil Henri, Prévost Gilles, Mourey Lionel

机构信息

Groupe de Biophysique Structurale, Département Mécanismes Moléculaires des Infections Mycobactériennes, CNRS-IPBS, 205 route de Narbonne, 31077 Toulouse Cedex, France.

出版信息

J Biol Chem. 2004 Sep 24;279(39):41028-37. doi: 10.1074/jbc.M406904200. Epub 2004 Jul 18.

Abstract

Staphylococcal leucocidins and gamma-hemolysins (leucotoxins) are bi-component toxins that form lytic transmembrane pores. Their cytotoxic activities require the synergistic association of a class S component and a class F component, produced as water-soluble monomers that form hetero-oligomeric membrane-associated complexes. Strains that produce the Panton-Valentine leucocidin are clinically associated with cutaneous lesions and community-acquired pneumonia. In a previous study, we determined the crystal structure of the F monomer from the Panton-Valentine leucocidin. To derive information on the second component of the leucotoxins, the x-ray structure of the S protein from the Panton-Valentine leucocidin was solved to 2.0 angstrom resolution using a tetragonal crystal form that contains eight molecules in the asymmetric unit. The structure demonstrates the different conformation of the domain involved in membrane contacts and illustrates sequence and tertiary structure variabilities of the pore-forming leucotoxins. Mutagenesis studies at a key surface residue (Thr-28) further support the important role played by these microheterogeneities for the assembly of the bipartite leucotoxins.

摘要

葡萄球菌杀白细胞素和γ-溶血素(白细胞毒素)是形成溶解性跨膜孔的双组分毒素。它们的细胞毒性活性需要S类组分和F类组分的协同结合,这两种组分以水溶性单体形式产生,形成异源寡聚体膜相关复合物。产生潘顿-瓦伦丁杀白细胞素的菌株在临床上与皮肤损伤和社区获得性肺炎有关。在先前的一项研究中,我们确定了潘顿-瓦伦丁杀白细胞素F单体的晶体结构。为了获得关于白细胞毒素第二种组分的信息,利用不对称单元中包含八个分子的四方晶型,将潘顿-瓦伦丁杀白细胞素S蛋白的X射线结构解析到2.0埃分辨率。该结构展示了参与膜接触的结构域的不同构象,并阐明了形成孔的白细胞毒素的序列和三级结构变异性。在一个关键表面残基(苏氨酸-28)处的诱变研究进一步支持了这些微观异质性在双组分白细胞毒素组装中所起的重要作用。

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