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纤连蛋白增强胎儿弯曲杆菌与细胞外基质成分及INT 407细胞的相互作用。

Fibronectin enhances Campylobacter fetus interaction with extracellular matrix components and INT 407 cells.

作者信息

Graham L L, Friel T, Woodman R L

机构信息

Department of Biology, St. Francis Xavier University, Antigonish, NS B2G2W5, Canada.

出版信息

Can J Microbiol. 2008 Jan;54(1):37-47. doi: 10.1139/w07-115.

Abstract

Campylobacter fetus is a recognized pathogen of cattle and sheep that can also infect humans. No adhesins specific for C. fetus have to date been identified; however, bacterial attachment is essential to establish an infecting population. Scanning electron microscopy revealed C. fetus attachment to the serosal surface of human colonic biopsy explants, a location consistent with the presence of the extracellular matrix (ECM). To determine whether the ECM mediated C. fetus adherence, 7 C. fetus strains were assessed in a solid-phase binding assay for their ability to bind to immobilized ECM components. Of the ECM components assayed, adherence to fibronectin was noted for all strains. Attachment to ECM components was neither correlated with S-layer expression nor with cell-surface hydrophobicity. Ligand immunoblots, however, identified the S-layer protein as a major site of fibronectin binding, and modified ECM binding assays revealed that soluble fibronectin significantly enhanced the attachment of S-layer-expressing C. fetus strains to other ECM components. Soluble fibronectin also increased C. fetus adherence to INT 407 cells. This adherence was inhibited when INT 407 cells were incubated with synthetic peptides containing an RGD sequence, indicating that integrin receptors were involved in fibronectin-mediated attachment. Together, this data suggests that C. fetus can bind to immobilized fibronectin and use soluble fibronectin to enhance attachment to other ECM components and intestinal epithelial cells. In vivo, fibronectin would promote bacterial adherence, thereby, contributing to the initial interaction of C. fetus with mucosal and submucosal surfaces.

摘要

胎儿弯曲杆菌是一种已被确认的牛羊病原体,也可感染人类。迄今为止,尚未鉴定出胎儿弯曲杆菌特有的黏附素;然而,细菌附着对于建立感染群体至关重要。扫描电子显微镜显示胎儿弯曲杆菌附着于人类结肠活检外植体的浆膜表面,该位置与细胞外基质(ECM)的存在一致。为了确定ECM是否介导胎儿弯曲杆菌的黏附,在固相结合试验中评估了7株胎儿弯曲杆菌菌株与固定化ECM成分结合的能力。在所检测的ECM成分中,所有菌株均显示出对纤连蛋白的黏附。对ECM成分的附着既与S层表达无关,也与细胞表面疏水性无关。然而,配体免疫印迹法确定S层蛋白是纤连蛋白结合的主要位点,改良的ECM结合试验表明,可溶性纤连蛋白显著增强了表达S层的胎儿弯曲杆菌菌株与其他ECM成分的附着。可溶性纤连蛋白还增加了胎儿弯曲杆菌对INT 407细胞的黏附。当INT 407细胞与含有RGD序列的合成肽一起孵育时,这种黏附受到抑制,表明整合素受体参与了纤连蛋白介导的附着。总之,这些数据表明胎儿弯曲杆菌可以结合固定化的纤连蛋白,并利用可溶性纤连蛋白增强与其他ECM成分和肠上皮细胞的附着。在体内,纤连蛋白会促进细菌黏附,从而有助于胎儿弯曲杆菌与黏膜和黏膜下表面的初始相互作用。

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