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首页> 外文期刊>Viruses >Identification and Characterization of Type IV Pili as the Cellular Receptor of Broad Host Range Stenotrophomonas maltophilia Bacteriophages DLP1 and DLP2
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Identification and Characterization of Type IV Pili as the Cellular Receptor of Broad Host Range Stenotrophomonas maltophilia Bacteriophages DLP1 and DLP2

机译:鉴定和表征IV型菌毛作为宽宿主范围嗜麦芽窄食单胞菌噬菌体DLP1和DLP2的细胞受体。

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Bacteriophages DLP1 and DLP2 are capable of infecting both Stenotrophomonas maltophilia and Pseudomonas aeruginosa strains, two highly antibiotic resistant bacterial pathogens, which is unusual for phages that typically exhibit extremely limited host range. To explain their unusual cross-order infectivity and differences in host range, we have identified the type IV pilus as the primary receptor for attachment. Screening of a P. aeruginosa PA01 mutant library, a host that is susceptible to DLP1 but not DLP2, identified DLP1-resistant mutants with disruptions in pilus structural and regulatory components. Subsequent complementation of the disrupted pilin subunit genes in PA01 restored DLP1 infection. Clean deletion of the major pilin subunit, pilA , in S. maltophilia strains D1585 and 280 prevented phage binding and lysis by both DLP1 and DLP2, and complementation restored infection by both. Transmission electron microscopy shows a clear interaction between DLP1 and pili of both D1585 and PA01. These results support the identity of the type IV pilus as the receptor for DLP1 and DLP2 infection across their broad host ranges. This research further characterizes DLP1 and DLP2 as potential “anti-virulence” phage therapy candidates for the treatment of multidrug resistant bacteria from multiple genera.
机译:噬菌体DLP1和DLP2能够感染嗜麦芽窄食单胞菌和铜绿假单胞菌菌株,这是两种高度抗生素抗性的细菌病原体,这对于通常表现出极为有限的宿主范围的噬菌体来说是罕见的。为了解释它们的非常规交叉感染性和宿主范围的差异,我们确定了IV型菌毛是附着的主要受体。铜绿假单胞菌PA01突变体文库(对DLP1敏感但对DLP2不敏感的宿主)的筛选确定了对菌毛结构和调控成分有破坏作用的DLP1抗性突变体。 PA01中被破坏的菌毛蛋白亚基基因的后续补充恢复了DLP1感染。嗜麦芽胞菌菌株D1585和280中主要菌毛蛋白亚基pilA的干净缺失阻止了DLP1和DLP2的噬菌体结合和裂解,并且互补作用恢复了两者的感染。透射电子显微镜显示D1585和PA01的DLP1和菌毛之间有明显的相互作用。这些结果支持IV型菌毛在其广泛宿主范围内作为DLP1和DLP2感染的受体的身份。这项研究进一步将DLP1和DLP2表征为潜在的“抗毒力”噬菌体治疗候选物,用于治疗来自多个属的耐多药细菌。

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