Pgf糖基化机制的翻译后修饰可调节变形链球菌OMZ175的生理和毒力。

IF 2.6 2区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular Microbiology Pub Date : 2024-08-01 Epub Date: 2023-11-16 DOI:10.1111/mmi.15190
Nicholas de Mojana di Cologna, Silke Andresen, Sandip Samaddar, Stephanie Archer-Hartmann, Ashley Marie Rogers, Jessica K Kajfasz, Tridib Ganguly, Bruna A Garcia, Irene Saengpet, Alexandra M Peterson, Parastoo Azadi, Christine M Szymanski, José A Lemos, Jacqueline Abranches
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引用次数: 0

摘要

变形链球菌通常与龋齿有关,形成生物膜的能力对其致病性至关重要。我们最近发现变形链球菌的Pgf糖基化机制,负责表面相关黏附素Cnm和WapA的翻译后修饰。由于四基因pgf操纵子(pgfS-pgfM1-pgfE-pgfM2)是S. mutans核心基因组的一部分,我们假设pgf系统的范围超出了Cnm和WapA糖基化。硅分析和tunicamycin敏感性试验表明Pgf机制和鼠李糖-葡萄糖多糖合成途径之间存在功能重叠。pgf突变体(ΔpgfS, ΔpgfE, ΔpgfM1, ΔpgfM2和Δpgf)的表型特征表明,pgf系统对人类唾液中生物膜的形成、表面电荷、膜稳定性和存活都很重要。此外,在大鼠口腔定植模型中,整个pgf操纵子(Δpgf菌株)的缺失导致定植明显受损。以Cnm为模型,我们发现Cnm被n -乙酰基己糖胺大量修饰,但随着PgfS糖基转移酶的失活,Cnm被大量磷酸化,这表明这两种翻译后修饰机制之间存在串扰。我们的研究结果表明,Pgf机制对变形链球菌病理生物学的多个方面都有贡献,可能超出了Cnm和WapA糖基化。
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Post-translational modification by the Pgf glycosylation machinery modulates Streptococcus mutans OMZ175 physiology and virulence.

Streptococcus mutans is commonly associated with dental caries and the ability to form biofilms is essential for its pathogenicity. We recently identified the Pgf glycosylation machinery of S. mutans, responsible for the post-translational modification of the surface-associated adhesins Cnm and WapA. Since the four-gene pgf operon (pgfS-pgfM1-pgfE-pgfM2) is part of the S. mutans core genome, we hypothesized that the scope of the Pgf system goes beyond Cnm and WapA glycosylation. In silico analyses and tunicamycin sensitivity assays suggested a functional overlap between the Pgf machinery and the rhamnose-glucose polysaccharide synthesis pathway. Phenotypic characterization of pgf mutants (ΔpgfS, ΔpgfE, ΔpgfM1, ΔpgfM2, and Δpgf) revealed that the Pgf system is important for biofilm formation, surface charge, membrane stability, and survival in human saliva. Moreover, deletion of the entire pgf operon (Δpgf strain) resulted in significantly impaired colonization in a rat oral colonization model. Using Cnm as a model, we showed that Cnm is heavily modified with N-acetyl hexosamines but it becomes heavily phosphorylated with the inactivation of the PgfS glycosyltransferase, suggesting a crosstalk between these two post-translational modification mechanisms. Our results revealed that the Pgf machinery contributes to multiple aspects of S. mutans pathobiology that may go beyond Cnm and WapA glycosylation.

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来源期刊
Molecular Microbiology
Molecular Microbiology 生物-生化与分子生物学
CiteScore
7.20
自引率
5.60%
发文量
132
审稿时长
1.7 months
期刊介绍: Molecular Microbiology, the leading primary journal in the microbial sciences, publishes molecular studies of Bacteria, Archaea, eukaryotic microorganisms, and their viruses. Research papers should lead to a deeper understanding of the molecular principles underlying basic physiological processes or mechanisms. Appropriate topics include gene expression and regulation, pathogenicity and virulence, physiology and metabolism, synthesis of macromolecules (proteins, nucleic acids, lipids, polysaccharides, etc), cell biology and subcellular organization, membrane biogenesis and function, traffic and transport, cell-cell communication and signalling pathways, evolution and gene transfer. Articles focused on host responses (cellular or immunological) to pathogens or on microbial ecology should be directed to our sister journals Cellular Microbiology and Environmental Microbiology, respectively.
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