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Isolation, characterization, therapeutic potential and depolymerase identification of a lytic bacteriophage Kpp-9 against Klebsiella pneumoniae with capsule serotype K2.

作者信息

Wang Menglu, Liu Jiayi, Jiao Xin, Liu Yanxia, Yang Shuqi, Gong Wenbin, Qiao Jinjuan

机构信息

Department of Medical Laboratory, Shandong Second Medical University, Weifang, Shandong, 261053, PR China.

Department of Basic Medicine, Weifang Nursing Vocational College, Weifang, Shandong, 262500, PR China.

出版信息

Microb Pathog. 2025 Nov;208:107950. doi: 10.1016/j.micpath.2025.107950. Epub 2025 Aug 5.

DOI:10.1016/j.micpath.2025.107950
PMID:40774563
Abstract

Klebsiella pneumoniae is one of the most threatening multidrug-resistant bacteria, and its inherent capsule and extensive biofilm formation pose a significant barrier to the treatment of infection. Bacteriophages (or phages) and phage-derived depolymerases are attracting attention as potential alternatives to antibiotics. Here, we isolated a lytic phage, named Kpp-9, using a capsule-type K2 strain, Kp09. Kpp-9 could inhibit bacterial biofilm formation, eradicate the mature biofilm in vitro, improve the survival rate of Kp09-infected mice, and alleviate the symptoms of pneumonia in mice. Morphological and genomic analyses showed that phage Kpp-9 belonged to the class Caudoviricetes and no virulence or resistance genes were found in the genome, indicating potential therapeutic applications of phage Kpp-9. Furthermore, two depolymerases (Kp9042 and Kp9050) were predicted and shown to be able to digest the capsule and improve the susceptibility of K. pneumoniae to complement-mediated serum killing. In addition, Kpp-9 and two depolymerases showed high selectivity for capsule-type K2 K. pneumoniae strains and exhibited robust thermal and pH stability. These results demonstrate that phage Kpp-9 and its encoded depolymerases Kp9042 and Kp9050 may serve as alternative therapeutic agents for the treatment of capsule-type K2 K. pneumoniae infections.

摘要

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