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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Design of a Broad-Range Bacteriophage Cocktail That Reduces Pseudomonas aeruginosa Biofilms and Treats Acute Infections in Two Animal Models
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Design of a Broad-Range Bacteriophage Cocktail That Reduces Pseudomonas aeruginosa Biofilms and Treats Acute Infections in Two Animal Models

机译:设计繁多的噬菌体鸡尾酒,可减少假单胞菌铜绿假单胞菌生物膜并治疗两种动物模型中的急性感染

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The alarming diffusion of multidrug-resistant (MDR) bacterial strains requires investigations on nonantibiotic therapies. Among such therapies, the use of bacteriophages (phages) as antimicrobial agents, namely, phage therapy, is a promising treatment strategy supported by the findings of recent successful compassionate treatments in Europe and the United States. In this work, we combined host range and genomic information to design a 6-phage cocktail killing several clinical strains of Pseudomonas aeruginosa, including those collected from Italian cystic fibrosis (CF) patients, and analyzed the cocktail performance. We demonstrated that the cocktail composed of four novel phages (PYO2, DEV, E215 and E217) and two previously characterized phages (PAK_P1 and PAK_P4) was able to lyse P. aeruginosa both in planktonic liquid cultures and in biofilms. In addition, we showed that the phage cocktail could cure acute respiratory infection in mice and treat bacteremia in wax moth (Galleria mellonella) larvae. Furthermore, administration of the cocktail to larvae prior to bacterial infection provided prophylaxis. In this regard, the efficiency of the phage cocktail was found to be unaffected by the MDR or mucoid phenotype of the pseudomonal strain. The cocktail was found to be superior to the individual phages in destroying biofilms and providing a faster treatment in mice. We also found the Galleria larva model to be cost-effective for testing the susceptibility of clinical strains to phages, suggesting that it could be implemented in the frame of developing personalized phage therapies.
机译:多药物抗性(MDR)细菌菌株的惊人扩散需要对非抗生素疗法的研究。在这种疗法中,使用噬菌体(噬菌体)作为抗微生物剂,即噬菌体疗法,是欧洲和美国最近成功的富有同情心的结果支持的有前途的治疗策略。在这项工作中,我们组合了主机范围和基因组信息,设计了6噬菌体鸡尾酒杀死几种临床菌株的铜绿假单胞菌,包括从意大利囊性纤维化(CF)患者收集的那些,并分析了鸡尾酒的性能。我们证明,由四种新噬菌体(PyO2,DeV,E215和E217)组成的鸡尾酒和两种先前表征的噬菌体(PAK_P1和PAK_P4)能够在浮鳞液体培养和生物膜中叙述铜绿假单胞菌。此外,我们表明,噬菌体鸡尾酒可以治愈小鼠急性呼吸道感染,治疗蜡蛾(Galleria Mellonella)幼虫的菌血症。此外,在细菌感染之前向幼虫施用鸡尾酒给幼虫提供预防。在这方面,发现噬菌体鸡尾酒的效率不受伪菌株的MDR或粘膜表型的影响。发现鸡尾酒在破坏生物膜和在小鼠中提供更快的治疗时,鸡尾酒优于各个噬菌体。我们还发现Galleria Larva模型对于测试临床菌株到噬菌体的敏感性,这表明它可以在开发个性化噬菌体疗法的框架中实施。

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