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唾液乳杆菌UCC118预测分泌蛋白组中sortase依赖性蛋白的比较与功能分析

Comparative and functional analysis of sortase-dependent proteins in the predicted secretome of Lactobacillus salivarius UCC118.

作者信息

van Pijkeren Jan-Peter, Canchaya Carlos, Ryan Kieran A, Li Yin, Claesson Marcus J, Sheil Barbara, Steidler Lothar, O'Mahony Liam, Fitzgerald Gerald F, van Sinderen Douwe, O'Toole Paul W

机构信息

Department of Microbiology, University College Cork, Cork, Ireland.

出版信息

Appl Environ Microbiol. 2006 Jun;72(6):4143-53. doi: 10.1128/AEM.03023-05.

Abstract

Surface proteins are important factors in the interaction of probiotic and pathogenic bacteria with their environment or host. We performed a comparative bioinformatic analysis of four publicly available Lactobacillus genomes and the genome of Lactobacillus salivarius subsp. salivarius strain UCC118 to identify secreted proteins and those linked to the cell wall. Proteins were identified which were predicted to be anchored by WXL-binding domains, N- or C-terminal anchors, GW repeats, lipoprotein anchors, or LysM-binding domains. We identified 10 sortase-dependent surface proteins in L. salivarius UCC118, including three which are homologous to mucus-binding proteins (LSL_0152, LSL_0311, and LSL_1335), a collagen-binding protein homologue (LSL_2020b), two hypothetical proteins (LSL_1838 and LSL_1902b), an enterococcal surface protein homologue (LSL_1085), a salivary agglutinin-binding homologue (LSL_1832b), an epithelial binding protein homologue (LSL_1319), and a proteinase homologue (LSL_1774b). However, two of the genes are gene fragments and four are pseudogenes, suggesting a lack of selection for their function. Two of the 10 genes were not transcribed in vitro, and 1 gene showed a 10-fold increase in transcript level in stationary phase compared to logarithmic phase. The sortase gene was deleted, and three genes encoding sortase-dependent proteins were disrupted. The sortase mutant and one sortase-dependent protein (mucus-binding homologue) mutant showed a significant reduction in adherence to human epithelial cell lines. The genome-wide investigation of surface proteins can thus help our understanding of their roles in host interaction.

摘要

表面蛋白是益生菌和病原菌与其环境或宿主相互作用的重要因素。我们对四个公开可用的乳酸杆菌基因组以及唾液乳杆菌唾液亚种UCC118的基因组进行了比较生物信息学分析,以鉴定分泌蛋白和与细胞壁相关的蛋白。鉴定出了预计通过WXL结合结构域、N端或C端锚定、GW重复序列、脂蛋白锚定或LysM结合结构域锚定的蛋白。我们在唾液乳杆菌UCC118中鉴定出10种分选酶依赖性表面蛋白,其中包括三种与黏液结合蛋白同源的蛋白(LSL_0152、LSL_0311和LSL_1335)、一种胶原结合蛋白同源物(LSL_2020b)、两种假定蛋白(LSL_1838和LSL_1902b)、一种肠球菌表面蛋白同源物(LSL_1085)、一种唾液凝集素结合同源物(LSL_1832b)、一种上皮结合蛋白同源物(LSL_1319)和一种蛋白酶同源物(LSL_1774b)。然而,其中两个基因是基因片段,四个是假基因,这表明对其功能缺乏选择。10个基因中有两个在体外未转录,1个基因在稳定期的转录水平比对数期增加了10倍。分选酶基因被删除,三个编码分选酶依赖性蛋白的基因被破坏。分选酶突变体和一种分选酶依赖性蛋白(黏液结合同源物)突变体对人上皮细胞系的黏附力显著降低。因此,对表面蛋白进行全基因组研究有助于我们了解它们在宿主相互作用中的作用。

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