Bacteriophages targeting Acinetobacter baumannii capsule induce antimicrobial resensitization

鲍曼不动杆菌 微生物学 溶解循环 生物 抗生素耐药性 抗菌剂 抗生素 细菌 噬菌体 噬菌体疗法 病毒学 基因 大肠杆菌 铜绿假单胞菌 病毒 遗传学
作者
Fernando Gordillo Altamirano,John H. Forsyth,Ruzeen Patwa,Xenia Kostoulias,Michael Trim,Dinesh Subedi,Stuart K. Archer,Faye C. Morris,Cody Oliveira,Luisa Kielty,Denis V. Korneev,Moira K. O’Bryan,Trevor Lithgow,Anton Y. Peleg,Jeremy J. Barr
标识
DOI:10.1101/2020.02.25.965590
摘要

Abstract Carbapenem-resistant Acinetobacter baumannii is responsible for frequent, hard-to-treat and often fatal healthcare-associated infections. Phage therapy, the use of viruses that infect and kill bacteria, is an approach gaining significant clinical interest to combat antibiotic-resistant infections. However, a major limitation is that bacteria can develop resistance against phages. Here, we isolated phages with activity against a panel of A. baumannii strains and focused on clinical isolates AB900 and A9844 and their phages for detailed characterization. As expected, coincubation of the phages with their hosts in vitro resulted in the emergence of phage-resistant bacterial mutants. Genome sequence analysis revealed that phage-resistant mutants harbored loss-of-function mutations in genes from the K locus, responsible for the biosynthesis of the bacterial capsule. Using molecular biology techniques, phage adsorption assays, and quantitative evaluation of capsule production, we established that the bacterial capsule serves as the primary receptor for these phages. As a collateral phenotype of impaired capsule production, the phage-resistant strains could not form biofilms, became fully sensitized to the human complement system, showed increased susceptibility to beta-lactam antibiotics, and became vulnerable to additional phages. Finally, in a murine model of bacteremia, the phage-resistant A. baumannii demonstrated a diminished capacity to colonize blood and solid tissues. This study demonstrates that phages can be used not only for their lytic activity but, if combined with a posteriori knowledge of their receptors and the mechanism of bacterial resistance, for their potential synergy with other antimicrobial agents, thus providing even broader clinical options for phage therapy.

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