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乙醇胺诱导的微区室组装是毒力所必需的。

Ethanolamine-induced assembly of microcompartments is required for virulence.

作者信息

Franklin Dana S, Chen Yi-Wei, Chen Yimin, Wittchen Manuel, Agnew Angela, Luu Alexis, Whitelegge Julian P, Zhou Z Hong, Tauch Andreas, Das Asis, Ton-That Hung

机构信息

Molecular Biology Institute, University of California, Los Angeles, California, USA.

Division of Oral & Systemic Health Sciences, School of Dentistry, University of California, Los Angeles, California, USA.

出版信息

mBio. 2025 Feb 5;16(2):e0340524. doi: 10.1128/mbio.03405-24. Epub 2024 Dec 23.

Abstract

UNLABELLED

Many bacteria metabolize ethanolamine as a nutrient source through cytoplasmic organelles named bacterial microcompartments (BMCs). Here we investigated the molecular assembly, regulation, and function of BMCs in a Gram-negative oral pathobiont that is associated with adverse pregnancy outcomes. The genome harbors a conserved ethanolamine utilization () locus with 21 genes that encode several putative BMC shell proteins and a two-component signal transduction system (TCS), in addition to the enzymes for ethanolamine transport and catabolism. We show that the expression of most of these genes and BMC formation are highly increased in wild-type fusobacteria when cultured in the presence of ethanolamine as a nutrient source. Deletion of the response regulator EutV eliminated this induction of mRNAs and BMCs, thus demonstrating that BMC formation is transcriptionally regulated by the TCS EutV-EutW in response to ethanolamine. Mass spectrometry of isolated BMCs unveiled the identity of the constituent proteins EutL, EutM, EutM, and EutN. Consistent with the role of these proteins in BMC assembly and metabolism, deletion of , //, or /// not only affected BMC formation but also ethanolamine utilization, causing cell growth defects with ethanolamine as a nutrient. BMCs are also assembled in fusobacteria cultured with placental cells or the culture media, a process that is dependent on the BMC shell proteins. Significantly, we show that the mutant is defective in inducing preterm birth in a mouse model. Together, these results establish that the BMC-mediated metabolism of ethanolamine is critical for fusobacterial virulence.

IMPORTANCE

The oral anaerobe can spread to distal internal organs, such as the colon and placenta, thereby promoting the development of colorectal cancer and inducing preterm birth, respectively. Yet, how this opportunistic pathogen adapts to the various metabolically distinct host cellular niches remains poorly understood. We demonstrated here that this microbe assembles specialized metabolic organelles, termed bacterial microcompartments (BMCs), to utilize environmental ethanolamine (EA) as a key environmental nutrient source. The formation of BMCs, containing BMC shell proteins EutLM1M2N, is controlled by a two-component system, EutV-EutW, responsive to EA. Significantly, this ability of to form BMCs in response to EA is crucial for its pathogenicity evidenced by the fact that the genetic disruption of BMC formation reduces fusobacterial virulence in a mouse model of preterm birth.

摘要

未标记

许多细菌通过名为细菌微区室(BMCs)的细胞质细胞器将乙醇胺作为营养源进行代谢。在此,我们研究了与不良妊娠结局相关的革兰氏阴性口腔致病共生菌中BMCs的分子组装、调控及功能。该基因组含有一个保守的乙醇胺利用()位点,有21个基因,除了编码乙醇胺转运和分解代谢的酶外,还编码几种假定的BMC外壳蛋白和一个双组分信号转导系统(TCS)。我们发现,当以乙醇胺作为营养源进行培养时,野生型梭杆菌中这些基因的大多数表达及BMC形成显著增加。应答调节因子EutV的缺失消除了这些mRNA和BMCs的诱导,从而证明BMC形成受TCS EutV - EutW转录调控以响应乙醇胺。对分离出的BMCs进行质谱分析揭示了组成蛋白EutL、EutM、EutM和EutN的身份。与这些蛋白在BMC组装和代谢中的作用一致,、//或///的缺失不仅影响BMC形成,还影响乙醇胺利用,导致以乙醇胺作为营养源时细胞生长缺陷。BMCs也在与胎盘细胞或培养基一起培养的梭杆菌中组装,这一过程依赖于BMC外壳蛋白。重要的是,我们表明突变体在小鼠模型中诱导早产存在缺陷。总之,这些结果表明BMC介导的乙醇胺代谢对梭杆菌毒力至关重要。

重要性

口腔厌氧菌可扩散至远端内部器官,如结肠和胎盘,从而分别促进结直肠癌的发展和诱导早产。然而,这种机会性病原体如何适应各种代谢不同的宿主细胞生态位仍知之甚少。我们在此证明,这种微生物组装了特殊的代谢细胞器,称为细菌微区室(BMCs),以利用环境乙醇胺(EA)作为关键的环境营养源。含有BMC外壳蛋白EutLM1M2N的BMCs的形成受双组分系统EutV - EutW控制,对EA有反应。重要的是,这种对EA响应形成BMCs的能力对其致病性至关重要,这一事实表明BMC形成的基因破坏会降低早产小鼠模型中的梭杆菌毒力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5896/11796344/60451184ede2/mbio.03405-24.f001.jpg

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