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BopA 对双歧双歧杆菌黏附于肠道上皮细胞、细胞外基质蛋白和黏液并无重要作用。

BopA does not have a major role in the adhesion of Bifidobacterium bifidum to intestinal epithelial cells, extracellular matrix proteins, and mucus.

机构信息

Department of Veterinary Biosciences, University of Helsinki, Helsinki, Finland.

出版信息

Appl Environ Microbiol. 2013 Nov;79(22):6989-97. doi: 10.1128/AEM.01993-13. Epub 2013 Sep 6.

Abstract

The ability of bifidobacteria to adhere to the intestine of the human host is considered to be important for efficient colonization and achieving probiotic effects. Bifidobacterium bifidum strains DSM20456 and MIMBb75 adhere well to the human intestinal cell lines Caco-2 and HT-29. The surface lipoprotein BopA was previously described to be involved in mediating adherence of B. bifidum to epithelial cells, but thioacylated, purified BopA inhibited the adhesion of B. bifidum to epithelial cells in competitive adhesion assays only at very high concentrations, indicating an unspecific effect. In this study, the role of BopA in the adhesion of B. bifidum was readdressed. The gene encoding BopA was cloned and expressed without its lipobox and hydrophobic signal peptide in Escherichia coli, and an antiserum against the recombinant BopA was produced. The antiserum was used to demonstrate the abundant localization of BopA on the cell surface of B. bifidum. However, blocking of B. bifidum BopA with specific antiserum did not reduce adhesion of bacteria to epithelial cell lines, arguing that BopA is not an adhesin. Also, adhesion of B. bifidum to human colonic mucin and fibronectin was found to be BopA independent. The recombinant BopA bound only moderately to human epithelial cells and colonic mucus, and it failed to bind to fibronectin. Thus, our results contrast the earlier findings on the major role of BopA in adhesion, indicating that the strong adhesion of B. bifidum to epithelial cell lines is BopA independent.

摘要

双歧杆菌黏附于人类宿主肠道的能力被认为是其有效定植和发挥益生菌作用的重要因素。双歧杆菌 Bifidobacterium bifidum 菌株 DSM20456 和 MIMBb75 能够很好地黏附于人类肠道细胞系 Caco-2 和 HT-29。先前的研究表明,表面脂蛋白 BopA 参与介导双歧杆菌黏附于肠上皮细胞,但硫代酰化的、纯化的 BopA 仅在非常高的浓度下才能抑制双歧杆菌在竞争黏附试验中与上皮细胞的黏附,表明这是一种非特异性的作用。在本研究中,重新研究了 BopA 在双歧杆菌黏附中的作用。克隆并在大肠杆菌中表达了无其脂质盒和疏水性信号肽的 BopA 基因,并制备了针对重组 BopA 的抗血清。该抗血清用于证明 BopA 在双歧杆菌表面的大量定位。然而,用特异性抗血清阻断双歧杆菌 BopA 并不能减少细菌对肠上皮细胞系的黏附,这表明 BopA 不是一种黏附素。此外,还发现双歧杆菌黏附于人结肠粘蛋白和纤维连接蛋白与 BopA 无关。重组 BopA 仅适度结合人上皮细胞和结肠黏液,并且不能结合纤维连接蛋白。因此,我们的研究结果与早期关于 BopA 在黏附中的主要作用的发现形成对比,表明双歧杆菌对肠上皮细胞系的强烈黏附与 BopA 无关。

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