Klebicin E, a pore-forming bacteriocin of Klebsiella pneumoniae, exploits the porin OmpC and the Ton system for translocation

细菌素 肺炎克雷伯菌 孔蛋白 生物 微生物学 毒素 细菌外膜 细菌 抗菌剂 大肠杆菌 生物化学 基因 遗传学
作者
Xinxin Zhao,Wenyu Wang,Xiaoli Zeng,Rong Xu,Bing Yuan,Wenyao Yu,Mingshu Wang,Renyong Jia,Shun Chen,Dekang Zhu,Mafeng Liu,Qiao Yang,Ying Wu,Shaqiu Zhang,Juan Huang,Xumin Ou,Di Sun,Anchun Cheng
出处
期刊:Journal of Biological Chemistry [Elsevier BV]
卷期号:300 (3): 105694-105694 被引量:1
标识
DOI:10.1016/j.jbc.2024.105694
摘要

Bacteriocins, which have narrow-spectrum activity and limited adverse effects, are promising alternatives to antibiotics. In this study, we identified klebicin E (KlebE), a small bacteriocin derived from Klebsiella pneumoniae. KlebE exhibited strong efficacy against multidrug-resistant K. pneumoniae isolates and conferred a significant growth advantage to the producing strain during intraspecies competition. A giant unilamellar vesicle leakage assay demonstrated the unique membrane permeabilization effect of KlebE, suggesting that it is a pore-forming toxin. In addition to a C-terminal toxic domain, KlebE also has a disordered N-terminal domain and a globular central domain. Pulldown assays and soft agar overlay experiments revealed the essential role of the outer membrane porin OmpC and the Ton system in KlebE recognition and cytotoxicity. Strong binding between KlebE and both OmpC and TonB was observed. The TonB-box, a crucial component of the toxin-TonB interaction, was identified as the 7-amino acid sequence (E3ETLTVV9) located in the N-terminal region. Further studies showed that a region near the bottom of the central domain of KlebE plays a primary role in recognizing OmpC, with eight residues surrounding this region identified as essential for KlebE toxicity. Finally, based on the discrepancies in OmpC sequences between the KlebE-resistant and sensitive strains, it was found that the 91st residue of OmpC, an aspartic acid residue, is a key determinant of KlebE toxicity. The identification and characterization of this toxin will facilitate the development of bacteriocin-based therapies targeting multidrug-resistant K. pneumoniae infections.
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