Mutation of wbtJ, a N-formyltransferase involved in O-antigen synthesis, results in biofilm formation, phase variation and attenuation in Francisella tularensis.

IF 2.6 4区 生物学 Q3 MICROBIOLOGY Microbiology-Sgm Pub Date : 2024-02-01 DOI:10.1099/mic.0.001437
Kevin D Mlynek, Ronald G Toothman, Elsie E Martinez, Ju Qiu, Joshua B Richardson, Joel A Bozue
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Abstract

Two clinically important subspecies, Francisella tularensis subsp. tularensis (type A) and F. tularensis subsp. holarctica (type B) are responsible for most tularaemia cases, but these isolates typically form a weak biofilm under in vitro conditions. Phase variation of the F. tularensis lipopolysaccharide (LPS) has been reported in these subspecies, but the role of variation is unclear as LPS is crucial for virulence. We previously demonstrated that a subpopulation of LPS variants can constitutively form a robust biofilm in vitro, but it is unclear whether virulence was affected. In this study, we show that biofilm-forming variants of both fully virulent F. tularensis subspecies were highly attenuated in the murine tularaemia model by multiple challenge routes. Genomic sequencing was performed on these strains, which revealed that all biofilm-forming variants contained a lesion within the wbtJ gene, a formyltransferase involved in O-antigen synthesis. A ΔwbtJ deletion mutant recapitulated the biofilm, O-antigen and virulence phenotypes observed in natural variants and could be rescued through complementation with a functional wbtJ gene. Since the spontaneously derived biofilm-forming isolates in this study were a subpopulation of natural variants, reversion events to the wbtJ gene were detected that eliminated the phenotypes associated with biofilm variants and restored virulence. These results demonstrate a role for WbtJ in biofilm formation, LPS variation and virulence of F. tularensis.

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wbtJ 是一种参与 O 抗原合成的 N-甲酰转移酶,它的突变会导致土拉弗氏菌生物膜的形成、阶段性变化和衰减。
两个临床上重要的亚种,即土拉菌弗朗西斯菌亚种(A 型)和土拉菌全株亚种(B 型)是大多数土拉菌病病例的罪魁祸首,但这些分离物在体外条件下通常会形成薄弱的生物膜。据报道,在这些亚种中,F. tularensis 脂多糖(LPS)发生了阶段性变异,但由于 LPS 对毒力至关重要,因此变异的作用尚不清楚。我们以前曾证明,LPS 变异亚群可在体外连续形成强大的生物膜,但尚不清楚毒力是否会受到影响。在本研究中,我们发现通过多种挑战途径,两种完全致病的 F. tularensis 亚种的生物膜形成变体在小鼠妥拉菌血症模型中都被高度减毒。对这些菌株进行了基因组测序,结果发现所有生物膜形成变种都含有一个 wbtJ 基因病变,该基因是一种参与 O 抗原合成的甲酰转移酶。ΔwbtJ缺失突变体再现了在天然变种中观察到的生物膜、O-抗原和毒力表型,并可通过与功能性 wbtJ 基因互补来挽救。由于本研究中自发产生的形成生物膜的分离株是天然变异株的一个亚群,因此检测到了 wbtJ 基因的还原事件,从而消除了与生物膜变异株相关的表型并恢复了毒力。这些结果证明了 WbtJ 在土拉菌的生物膜形成、LPS 变异和毒力中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Microbiology-Sgm
Microbiology-Sgm 生物-微生物学
CiteScore
4.60
自引率
7.10%
发文量
132
审稿时长
3.0 months
期刊介绍: We publish high-quality original research on bacteria, fungi, protists, archaea, algae, parasites and other microscopic life forms. Topics include but are not limited to: Antimicrobials and antimicrobial resistance Bacteriology and parasitology Biochemistry and biophysics Biofilms and biological systems Biotechnology and bioremediation Cell biology and signalling Chemical biology Cross-disciplinary work Ecology and environmental microbiology Food microbiology Genetics Host–microbe interactions Microbial methods and techniques Microscopy and imaging Omics, including genomics, proteomics and metabolomics Physiology and metabolism Systems biology and synthetic biology The microbiome.
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