Emerging Microbes and Infections (Dec 2022)

Interactions between host epithelial cells and Acinetobacter baumannii promote the emergence of highly antibiotic resistant and highly mucoid strains

  • Wang Zhang,
  • Yue Yao,
  • Hua Zhou,
  • Jintao He,
  • Jingfen Wang,
  • Li Li,
  • Minsong Gao,
  • Xiaochen Liu,
  • Ya Shi,
  • Jinzhong Lin,
  • Jianzhao Liu,
  • Huan Chen,
  • Yu Feng,
  • Zhihui Zhou,
  • Yunsong Yu,
  • Xiaoting Hua

DOI
https://doi.org/10.1080/22221751.2022.2136534
Journal volume & issue
Vol. 11, no. 1
pp. 2556 – 2569

Abstract

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Acinetobacter baumannii is an important nosocomial pathogen. Upon colonizing a host, A. baumannii are subjected to selective pressure by immune defenses as they adapt to the host environment. However, the mechanism of this pathoadaptation is unknown. Here, we established an in vitro system to evolve A. baumannii driven by the continuous selective pressure exerted by epithelial cells, and we used a combination of experimental evolution, phenotypic characterization and multi-omics analysis to address the underlying mechanism. When continuously exposed to selective pressure by pulmonary epithelial cells, A. baumannii showed ptk mutation-mediated mucoid conversion (reduced adhesion and increased anti-phagocytic ability) by enhancement of capsular exopolysaccharide chain length; rsmG mutation-mediated deficiency of 7-methylguanosine modification in the 524th nucleotide of 16S rRNA, which increased ribosome translation efficiency; and rnaseI mutation-mediated changes in outer membrane permeability and efflux pump expression. Together, these mutations altered susceptibility to a variety of antimicrobial agents, including the novel antibiotic cefiderocol, by regulating siderophore and siderophore-receptor biosynthesis. In conclusion, pulmonary epithelial cells modulate A. baumannii pathoadaptation, implicating the host–microbe interaction in the survival and persistence of A. baumannii.

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