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Combining Whole-Genome Sequencing and Multimodel Phenotyping To Identify Genetic Predictors of Salmonella Virulence

机译:结合全基因组测序和多模胞表型鉴定沙门氏菌毒力的遗传预测因子

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Salmonella comprises more than 2,600 serovars. Very few environmental and uncommon serovars have been characterized for their potential role in virulence and human infections. A complementary in vitro and in vivo systematic high-throughput analysis of virulence was used to elucidate the association between genetic and phenotypic variations across Salmonella isolates. The goal was to develop a strategy for the classification of isolates as a benchmark and predict virulence levels of isolates. Thirty-five phylogenetically distant strains of unknown virulence were selected from the Salmonella Foodborne Syst-OMICS (SalFoS) collection, representing 34 different serovars isolated from various sources. Isolates were evaluated for virulence in 4 complementary models of infection to compare virulence traits with the genomics data, including interactions with human intestinal epithelial cells, human macrophages, and amoeba. In vivo testing was conducted using the mouse model of Salmonella systemic infection. Significant correlations were identified between the different models. We identified a collection of novel hypothetical and conserved proteins associated with isolates that generate a high burden. We also showed that blind prediction of virulence of 33 additional strains based on the pan-genome was high in the mouse model of systemic infection (82% agreement) and in the human epithelial cell model (74% agreement). These complementary approaches enabled us to define virulence potential in different isolates and present a novel strategy for risk assessment of specific strains and for better monitoring and source tracking during outbreaks. IMPORTANCE Salmonella species are bacteria that are a major source of foodborne disease through contamination of a diversity of foods, including meat, eggs, fruits, nuts, and vegetables. More than 2,600 different Salmonella enterica serovars have been identified, and only a few of them are associated with illness in humans. Despite the fact that they are genetically closely related, there is enormous variation in the virulence of different isolates of Salmonella enterica . Identification of foodborne pathogens is a lengthy process based on microbiological, biochemical, and immunological methods. Here, we worked toward new ways of integrating whole-genome sequencing (WGS) approaches into food safety practices. We used WGS to build associations between virulence and genetic diversity within 83 Salmonella isolates representing 77 different Salmonella serovars. Our work demonstrates the potential of combining a genomics approach and virulence tests to improve the diagnostics and assess risk of human illness associated with specific Salmonella isolates.
机译:Salmonella包含2,600多台塞洛瓦。很少有环境和罕见的塞洛瓦斯的特征在于它们在毒力和人类感染中的潜在作用。使用体外和体内体内系统高通量分析的互补性用于阐明沙门氏菌分离株的遗传和表型变化之间的关联。目标是制定分离株作为基准和预测分离株的毒力水平的策略。从沙门氏菌食品载体系统中选择了35个神经发生的神经静脉曲张的菌株,代表了从各种来源中分离的34种不同的血清素。在4个互补模型中评估分离物的毒力,以比较具有基因组学数据的毒力性状,包括与人类肠上皮细胞,人巨噬细胞和AmoEba的相互作用。使用Salmonella系统性感染的小鼠模型进行体内测试。不同模型之间识别出显着的相关性。我们确定了与产生高负荷的分离物相关的新型假想和保守蛋白质的集合。我们还表明,基于泛基因组的33种额外菌株的毒力的盲预测在全身性感染(82%协议)和人上皮细胞模型(74%协议)中具有高毒性。这些互补方法使我们能够定义不同分离物中的毒力潜力,并提出了一种新的特定菌株风险评估的新策略以及在爆发期间更好的监测和源跟踪。 Importance Salmonella物种是通过污染食物的多样性,包括肉类,鸡蛋,水果,坚果和蔬菜,是食物中疾病的主要来源。已经确定了超过2,600种不同的沙门氏菌肠道肠道塞洛维尔,其中少数人与人类的疾病有关。尽管它们是转基因密切相关的事实,但沙门氏菌的不同分离株的毒力存在巨大变化。鉴定食品载体病原体是基于微生物,生物化学和免疫学方法的冗长过程。在这里,我们致力于将全基因组测序(WGS)方法集成到食品安全实践中的新方法。我们使用WGS在83个沙门氏菌中的毒力和遗传多样性之间建立关联,该分离物代表77种不同的沙门氏菌塞洛维拉斯。我们的作品展示了结合基因组学方法和毒力试验的潜力,以改善诊断和评估与特定沙门氏菌的人类疾病的风险。

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