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与毒力相关的丝状噬菌体MDAΦ的结构

Structure of the virulence-associated filamentous bacteriophage MDAΦ.

作者信息

Böhning Jan, Graham Miles, Coureuil Mathieu, Tarafder Abul K, Meyer Julie, Nassif Xavier, Bille Emmanuelle, Bharat Tanmay A M

机构信息

Structural Studies Division, Medical Research Council Laboratory of Molecular Biology, Cambridge CB2 0QH, United Kingdom.

INSERM U1151, CNRS UMR8253, Institut Necker-Enfants Malades, Université Paris Cité, Paris F-75015, France.

出版信息

Proc Natl Acad Sci U S A. 2025 Jun 24;122(25):e2420157122. doi: 10.1073/pnas.2420157122. Epub 2025 Jun 20.

Abstract

is a human commensal bacterium that can opportunistically invade the bloodstream and cross the blood-brain barrier, where it can cause septicemia and meningitis. These diseases, if left untreated, can be lethal within hours. Hyperinvasive strains often express a genomically encoded filamentous bacteriophage called MDAΦ, which promotes colonization of mucosal host surfaces to facilitate bacterial invasion. How this phage is organized and how it promotes biofilm formation and infection at the molecular level is unclear. Here, we present an electron cryomicroscopy structure of the MDA phage, showing that MDAΦ is a class I filamentous inovirus, with the major capsid protein (MCP) arranged within the phage as a highly curved and densely packed α-helix. Comparison with other filamentous bacteriophages offers clues about inoviral genome encapsidation mechanisms, providing a framework for understanding the evolutionary diversity of inoviruses. A disordered, N-terminal segment in the MCP presents hydrophobic patches on the surface of assembled phage particles, which, together with electron cryotomography data of phage bundles, furnishes a structural rationale for phage-phage interactions that were seen previously in an epithelium adhesion infection model of . Taken together, our results shed light on the structure, organization, and higher-order assembly of a biomedically relevant phage encoded in the genome of a human pathogen. Molecular insights gleaned from this study increase our understanding of phage evolution, phage-mediated bacterial adhesion, and pathogenicity.

摘要

是一种人体共生细菌,可伺机侵入血流并穿越血脑屏障,在那里可导致败血症和脑膜炎。这些疾病若不治疗,数小时内即可致命。高侵袭性菌株通常表达一种基因组编码的丝状噬菌体,称为MDAΦ,它促进在粘膜宿主表面的定殖,以利于细菌入侵。这种噬菌体如何组装以及它如何在分子水平上促进生物膜形成和感染尚不清楚。在这里,我们展示了MDA噬菌体的电子冷冻显微镜结构,表明MDAΦ是一种I类丝状肌病毒,主要衣壳蛋白(MCP)在噬菌体中排列成高度弯曲且紧密堆积的α螺旋。与其他丝状噬菌体的比较提供了关于肌病毒基因组包装机制的线索,为理解肌病毒的进化多样性提供了一个框架。MCP中一个无序的N端片段在组装的噬菌体颗粒表面呈现疏水斑块,这与噬菌体束的电子冷冻断层扫描数据一起,为先前在一种上皮粘附感染模型中观察到的噬菌体-噬菌体相互作用提供了结构原理。综上所述,我们的结果揭示了一种人类病原体基因组中编码的具有生物医学相关性的噬菌体的结构、组装和高阶组装。从这项研究中获得的分子见解增进了我们对噬菌体进化、噬菌体介导的细菌粘附和致病性的理解。

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