Heterologous Expression of a Cryptic BGC from Bilophila sp. Provides Access to a Novel Family of Antibacterial Thiazoles.

IF 3.7 2区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS
ACS Synthetic Biology Pub Date : 2025-03-21 Epub Date: 2025-02-25 DOI:10.1021/acssynbio.5c00042
Maximilian Hohmann, Denis Iliasov, Martin Larralde, Widya Johannes, Klaus-Peter Janßen, Georg Zeller, Thorsten Mascher, Tobias A M Gulder
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引用次数: 0

Abstract

Human health is greatly influenced by the gut microbiota and microbiota imbalance can lead to the development of diseases. It is widely acknowledged that the interaction of bacteria within competitive ecosystems is influenced by their specialized metabolites, which act, e.g., as antibacterials or siderophores. However, our understanding of the occurrence and impact of such natural products in the human gut microbiome remains very limited. As arylthiazole siderophores are an emerging family of growth-promoting molecules in pathogenic bacteria, we analyzed a metagenomic data set from the human microbiome and thereby identified the bil-BGC, which originates from an uncultured Bilophila strain. Through gene synthesis and BGC assembly, heterologous expression and mutasynthetic experiments, we discovered the arylthiazole natural products bilothiazoles A-F. While established activities of related molecules indicate their involvement in metal-binding and -uptake, which could promote the growth of pathogenic strains, we also found antibiotic activity for some bilothiazoles. This is supported by biosensor-experiments, where bilothiazoles C and E show PrecA-suppressing activity, while bilothiazole F induces PblaZ, a biosensor characteristic for β-lactam antibiotics. These findings serve as a starting point for investigating the role of bilothiazoles in the pathogenicity of Bilophila species in the gut.

来自Bilophila sp.的一个隐性BGC的异源表达提供了一个新的抗菌噻唑家族的途径。
人体健康受到肠道菌群的极大影响,菌群失衡可导致疾病的发展。人们普遍认为,竞争生态系统内细菌的相互作用受到它们的特殊代谢物的影响,这些代谢物的作用,例如,作为抗菌剂或铁载体。然而,我们对这些天然产物在人类肠道微生物群中的发生和影响的了解仍然非常有限。由于芳基噻唑铁载体是致病菌中一个新兴的促进生长的分子家族,我们分析了来自人类微生物组的宏基因组数据集,从而确定了bill - bgc,它起源于未培养的Bilophila菌株。通过基因合成、BGC组装、异源表达、突变合成等实验,发现了芳基噻唑类天然产物双噻唑A-F。虽然相关分子的活性表明它们参与金属结合和摄取,从而促进致病菌株的生长,但我们也发现了一些双噻唑类药物的抗生素活性。这得到了生物传感器实验的支持,在实验中,十二噻唑C和E显示出preca抑制活性,而十二噻唑F诱导PblaZ,这是一种β-内酰胺类抗生素的生物传感器特征。这些发现可作为研究双噻唑在肠道嗜杆菌致病性中的作用的起点。
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来源期刊
CiteScore
8.00
自引率
10.60%
发文量
380
审稿时长
6-12 weeks
期刊介绍: The journal is particularly interested in studies on the design and synthesis of new genetic circuits and gene products; computational methods in the design of systems; and integrative applied approaches to understanding disease and metabolism. Topics may include, but are not limited to: Design and optimization of genetic systems Genetic circuit design and their principles for their organization into programs Computational methods to aid the design of genetic systems Experimental methods to quantify genetic parts, circuits, and metabolic fluxes Genetic parts libraries: their creation, analysis, and ontological representation Protein engineering including computational design Metabolic engineering and cellular manufacturing, including biomass conversion Natural product access, engineering, and production Creative and innovative applications of cellular programming Medical applications, tissue engineering, and the programming of therapeutic cells Minimal cell design and construction Genomics and genome replacement strategies Viral engineering Automated and robotic assembly platforms for synthetic biology DNA synthesis methodologies Metagenomics and synthetic metagenomic analysis Bioinformatics applied to gene discovery, chemoinformatics, and pathway construction Gene optimization Methods for genome-scale measurements of transcription and metabolomics Systems biology and methods to integrate multiple data sources in vitro and cell-free synthetic biology and molecular programming Nucleic acid engineering.
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