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Molecular Characterization of Host-Specific Biofilm Formation in a Vertebrate Gut Symbiont

机译:脊椎动物肠道共生体中特定于宿主生物膜形成的分子表征。

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摘要

Although vertebrates harbor bacterial communities in their gastrointestinal tract whose composition is host-specific, little is known about the mechanisms by which bacterial lineages become selected. The goal of this study was to characterize the ecological processes that mediate host-specificity of the vertebrate gut symbiont Lactobacillus reuteri, and to systematically identify the bacterial factors that are involved. Experiments with monoassociated mice revealed that the ability of L. reuteri to form epithelial biofilms in the mouse forestomach is strictly dependent on the strain's host origin. To unravel the molecular basis for this host-specific biofilm formation, we applied a combination of transcriptome analysis and comparative genomics and identified eleven genes of L. reuteri 100-23 that were predicted to play a role. We then determined expression and importance of these genes during in vivo biofilm formation in monoassociated mice. This analysis revealed that six of the genes were upregulated in vivo, and that genes encoding for proteins involved in epithelial adherence, specialized protein transport, cell aggregation, environmental sensing, and cell lysis contributed to biofilm formation. Inactivation of a serine-rich surface adhesin with a devoted transport system (the SecA2-SecY2 pathway) completely abrogated biofilm formation, indicating that initial adhesion represented the most significant step in biofilm formation, likely conferring host specificity. In summary, this study established that the epithelial selection of bacterial symbionts in the vertebrate gut can be both specific and highly efficient, resulting in biofilms that are exclusively formed by the coevolved strains, and it allowed insight into the bacterial effectors of this process.
机译:尽管脊椎动物在其胃肠道中具有细菌寄主群落,而细菌群落的组成是宿主特异性的,但对于细菌谱系选择的机制知之甚少。这项研究的目的是表征介导脊椎动物肠道共生体罗伊氏乳杆菌的宿主特异性的生态过程,并系统地鉴定涉及的细菌因子。单关联小鼠的实验表明罗伊氏乳杆菌在小鼠前胃中形成上皮生物膜的能力严格取决于菌株的宿主来源。为了弄清这种宿主特异性生物膜形成的分子基础,我们结合了转录组分析和比较基因组学方法,确定了预计将发挥作用的罗伊氏乳杆菌100-23的十一个基因。然后,我们确定了在单个相关小鼠体内生物膜形成过程中这些基因的表达和重要性。该分析揭示了其中的六个基因在体内被上调,并且编码参与上皮粘附,专门的蛋白质转运,细胞聚集,环境传感和细胞裂解的蛋白质的基因促成了生物膜的形成。通过专用的转运系统(SecA2-SecY2途径)使富含丝氨酸的表面粘附素失活,从而完全消除了生物膜的形成,表明初始粘附代表了生物膜形成中最重要的一步,可能赋予了宿主特异性。总而言之,这项研究确定了脊椎动物肠道中细菌共生菌的上皮选择既可以是特异性的,又可以是高效的,从而导致生物膜仅由共同进化的菌株形成,并且可以深入了解这一过程的细菌效应子。

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