A genome-scale metabolic model of a globally disseminated hyperinvasive M1 strain of Streptococcus pyogenes.

IF 5 2区 生物学 Q1 MICROBIOLOGY
mSystems Pub Date : 2024-09-17 Epub Date: 2024-08-19 DOI:10.1128/msystems.00736-24
Yujiro Hirose, Daniel C Zielinski, Saugat Poudel, Kevin Rychel, Jonathon L Baker, Yoshihiro Toya, Masaya Yamaguchi, Almut Heinken, Ines Thiele, Shigetada Kawabata, Bernhard O Palsson, Victor Nizet
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引用次数: 0

Abstract

Streptococcus pyogenes is responsible for a range of diseases in humans contributing significantly to morbidity and mortality. Among more than 200 serotypes of S. pyogenes, serotype M1 strains hold the greatest clinical relevance due to their high prevalence in severe human infections. To enhance our understanding of pathogenesis and discovery of potential therapeutic approaches, we have developed the first genome-scale metabolic model (GEM) for a serotype M1 S. pyogenes strain, which we name iYH543. The curation of iYH543 involved cross-referencing a draft GEM of S. pyogenes serotype M1 from the AGORA2 database with gene essentiality and autotrophy data obtained from transposon mutagenesis-based and growth screens. We achieved a 92.6% (503/543 genes) accuracy in predicting gene essentiality and a 95% (19/20 amino acids) accuracy in predicting amino acid auxotrophy. Additionally, Biolog Phenotype microarrays were employed to examine the growth phenotypes of S. pyogenes, which further contributed to the refinement of iYH543. Notably, iYH543 demonstrated 88% accuracy (168/190 carbon sources) in predicting growth on various sole carbon sources. Discrepancies observed between iYH543 and the actual behavior of living S. pyogenes highlighted areas of uncertainty in the current understanding of S. pyogenes metabolism. iYH543 offers novel insights and hypotheses that can guide future research efforts and ultimately inform novel therapeutic strategies.IMPORTANCEGenome-scale models (GEMs) play a crucial role in investigating bacterial metabolism, predicting the effects of inhibiting specific metabolic genes and pathways, and aiding in the identification of potential drug targets. Here, we have developed the first GEM for the S. pyogenes highly virulent serotype, M1, which we name iYH543. The iYH543 achieved high accuracy in predicting gene essentiality. We also show that the knowledge obtained by substituting actual measurement values for iYH543 helps us gain insights that connect metabolism and virulence. iYH543 will serve as a useful tool for rational drug design targeting S. pyogenes metabolism and computational screening to investigate the interplay between inhibiting virulence factor synthesis and growth.

全球传播的高侵袭性化脓性链球菌 M1 株的基因组尺度代谢模型。
化脓性链球菌是人类一系列疾病的元凶,严重影响发病率和死亡率。在 200 多种化脓性链球菌血清型中,血清型 M1 菌株因其在严重人类感染中的高流行率而具有最大的临床意义。为了加深我们对致病机理的了解并发现潜在的治疗方法,我们为血清型 M1 化脓性链球菌菌株开发了首个基因组尺度代谢模型(GEM),并将其命名为 iYH543。iYH543 的制作包括将 AGORA2 数据库中的 M1 血清型化脓性链球菌 GEM 草案与基于转座子诱变和生长筛选获得的基因本质和自营养数据进行交叉比对。我们预测基因本质的准确率为 92.6%(503/543 个基因),预测氨基酸营养不良的准确率为 95%(19/20 个氨基酸)。此外,我们还利用 Biolog 表型微阵列检测了化脓性链球菌的生长表型,这进一步促进了 iYH543 的完善。值得注意的是,iYH543 在预测各种唯一碳源上的生长时显示出 88% 的准确率(168/190 碳源)。重要意义基因组尺度模型(GEM)在研究细菌代谢、预测抑制特定代谢基因和途径的效果以及帮助鉴定潜在药物靶点方面发挥着至关重要的作用。在这里,我们开发了第一个针对化脓性链球菌高致病性血清型 M1 的 GEM,并将其命名为 iYH543。iYH543 在预测基因本质方面达到了很高的准确度。我们还表明,用实际测量值代替 iYH543 所获得的知识有助于我们深入了解新陈代谢与毒力之间的关系。iYH543 将成为针对化脓性链球菌新陈代谢的合理药物设计和计算筛选的有用工具,以研究抑制毒力因子合成与生长之间的相互作用。
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
mSystems
mSystems Biochemistry, Genetics and Molecular Biology-Biochemistry
CiteScore
10.50
自引率
3.10%
发文量
308
审稿时长
13 weeks
期刊介绍: mSystems™ will publish preeminent work that stems from applying technologies for high-throughput analyses to achieve insights into the metabolic and regulatory systems at the scale of both the single cell and microbial communities. The scope of mSystems™ encompasses all important biological and biochemical findings drawn from analyses of large data sets, as well as new computational approaches for deriving these insights. mSystems™ will welcome submissions from researchers who focus on the microbiome, genomics, metagenomics, transcriptomics, metabolomics, proteomics, glycomics, bioinformatics, and computational microbiology. mSystems™ will provide streamlined decisions, while carrying on ASM''s tradition of rigorous peer review.
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