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Cell Surface-Associated Elongation Factor Tu Mediates the Attachment of Lactobacillus johnsonii NCC533 (La1) to Human Intestinal Cells and Mucins

机译:细胞表面相关的延伸因子Tu介导约翰逊乳杆菌NCC533(La1)对人体肠道细胞和粘蛋白的附着。

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摘要

The aim of this work was to identify Lactobacillus johnsonii NCC533 (La1) surface molecules mediating attachment to intestinal epithelial cells and mucins. Incubation of Caco-2 intestinal epithelial cells with an L. johnsonii La1 cell wall extract led to the recognition of elongation factor Tu (EF-Tu) as a novel La1 adhesin-like factor. The presence of EF-Tu at the surface of La1 was confirmed by analysis of purified outer surface protein extract by immunoblotting experiments, by electron microscopy, and by enzyme-linked immunosorbent assays of live bacteria. Furthermore, tandem mass spectrometry analysis proved that EF-TU was expressed at the La1 surface as an intact molecule. Using recombinant La1 EF-Tu protein, we were able to determine that its binding to intestinal cells and to mucins is pH dependent. Competition experiments suggested that EF-Tu has an important role in La1 mucin binding capacity. In addition, immunomodulation studies performed on HT29 cells showed that EF-Tu recombinant protein can induce a proinflammatory response in the presence of soluble CD14. Our in vitro results indicate that EF-Tu, through its binding to the intestinal mucosa, might participate in gut homeostasis.
机译:这项工作的目的是确定介导约翰逊乳杆菌NCC533(La1)表面分子介导对肠上皮细胞和粘蛋白的附着。 C. 2肠上皮细胞与约翰逊乳杆菌La1细胞壁提取物的孵育导致将延伸因子Tu(EF-Tu)识别为一种新型的La1粘附素样因子。通过免疫印迹实验,电子显微镜和活菌的酶联免疫吸附试验分析纯化的外表面蛋白提取物,证实了La1表面上EF-Tu的存在。此外,串联质谱分析证明EF-TU作为完整分子在La1表面表达。使用重组La1 EF-Tu蛋白,我们能够确定其与肠细胞和粘蛋白的结合是pH依赖性的。竞争实验表明,EF-Tu在La1粘蛋白结合能力中具有重要作用。此外,对HT29细胞进行的免疫调节研究表明,在可溶性CD14存在下,EF-Tu重组蛋白可诱导促炎反应。我们的体外结果表明,EF-Tu通过与肠粘膜结合,可能参与肠道稳态。

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