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Dolosigranulum pigrum Cooperation and Competition in Human Nasal Microbiota

机译:Dolosigranulum PIGRUM合作与人类鼻腔微生物群的竞争

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Multiple epidemiological studies identify Dolosigranulum pigrum as a candidate beneficial bacterium based on its positive association with health, including negative associations with nasal/nasopharyngeal colonization by the pathogenic species Staphylococcus aureus and Streptococcus pneumoniae . Using a multipronged approach to gain new insights into D. pigrum function, we observed phenotypic interactions and predictions of genomic capacity that support the idea of a role for microbe-microbe interactions involving D. pigrum in shaping the composition of human nasal microbiota. We identified in vivo community-level and in vitro phenotypic cooperation by specific nasal Corynebacterium species. Also, D. pigrum inhibited S. aureus growth in vitro , whereas robust inhibition of S. pneumoniae required both D. pigrum and a nasal Corynebacterium together. D. pigrum l -lactic acid production was insufficient to account for these inhibitions. Genomic analysis of 11 strains revealed that D. pigrum has a small genome (average 1.86?Mb) and multiple predicted auxotrophies consistent with D. pigrum relying on its human host and on cocolonizing bacteria for key nutrients. Further, the accessory genome of D. pigrum harbored a diverse repertoire of biosynthetic gene clusters, some of which may have a role in microbe-microbe interactions. These new insights into D. pigrum ’s functions advance the field from compositional analysis to genomic and phenotypic experimentation on a potentially beneficial bacterial resident of the human upper respiratory tract and lay the foundation for future animal and clinical experiments. IMPORTANCE Staphylococcus aureus and Streptococcus pneumoniae infections cause significant morbidity and mortality in humans. For both, nasal colonization is a risk factor for infection. Studies of nasal microbiota identify Dolosigranulum pigrum as a benign bacterium present when adults are free of S. aureus or when children are free of S. pneumoniae . Here, we validated these in vivo associations with functional assays. We found that D. pigrum inhibited S. aureus in vitro and, together with a specific nasal Corynebacterium species, also inhibited S. pneumoniae . Furthermore, genomic analysis of D. pigrum indicated that it must obtain key nutrients from other nasal bacteria or from humans. These phenotypic interactions support the idea of a role for microbe-microbe interactions in shaping the composition of human nasal microbiota and implicate D. pigrum as a mutualist of humans. These findings support the feasibility of future development of microbe-targeted interventions to reshape nasal microbiota composition to exclude S. aureus and/or S. pneumoniae .
机译:多个流行病学研究确定Dolosigranulum pigrum基于健康的正相关的候选有益细菌,包括由致病菌种金黄色葡萄球菌和肺炎链球菌鼻/鼻咽定植负面的联想。使用多管齐下,以获得新的见解D. pigrum功能,我们观察到的表型相互作用和基因组的预测能力,支持对涉及D. pigrum在塑造人的鼻腔菌群的组成微生物微生物相互作用角色的想法。我们体内社区级和由具体的鼻棒状杆菌属体外表型鉴定的合作。此外,D. pigrum在体外抑制金黄色葡萄球菌的生长,而肺炎链球菌的鲁棒抑制所需既D. pigrum和鼻棒状杆菌在一起。 D. pigrum L-乳酸生产不足以帐户这些压抑。 11株的基因组分析表明,D. pigrum有一个小的基因组(平均1.86?MB)和多预测营养缺陷与D. pigrum依靠其人力主机和cocolonizing细菌主要营养素是一致的。此外,D. pigrum的附件基因组窝藏生物合成基因簇,其中的一些可以具有微生物微生物相互作用中起作用的不同组成部分。这些新的见解D. pigrum的功能,推进对人体上呼吸道的潜在有益细菌居民从成分分析基因组和表型的实验领域,并为未来的动物和临床实验奠定了基础。重要性金黄色葡萄球菌和肺炎链球菌感染引起人类显著的发病率和死亡率。对于这两种,鼻建群是感染的危险因素。鼻菌群的研究确定Dolosigranulum pigrum为良性细菌存在时大人是免费的金黄色葡萄球菌或当孩子是免费的肺炎链球菌。在这里,我们体内协会与功能分析验证这些。我们发现D. pigrum抑制金黄色葡萄球菌在体外,并与特定的鼻棒状杆菌属,也抑制了肺炎链球菌在一起。此外,D pigrum的基因组分析表明,它必须从其他鼻腔细菌或由人体重要的营养素。这些表型的交互支持微生物微生物相互作用角色的想法在塑造人的鼻腔菌群和株连D. pigrum的组成与人类的互助。这些发现支持微生物有针对性的干预未来发展的可行性,以重塑鼻菌群组成,以排除金黄色葡萄球菌和/或肺炎链球菌。

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