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Dual role of the colonization factor CD2831 in Clostridium difficile pathogenesis

机译:结肠因子CD2831在梭菌艰难梭菌性发病机制中的双重作用

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Clostridium difficile is a Gram-positive, anaerobic bacterium and the leading cause of antibiotic-associated diarrhea and pseudomembranous colitis. C. difficile modulates its transition from a motile to a sessile lifestyle through a mechanism of riboswitches regulated by cyclic diguanosine monophosphate (c-di-GMP). Previously described as a sortase substrate positively regulated by c-di-GMP, CD2831 was predicted to be a collagen-binding protein and thus potentially involved in sessility. By overexpressing CD2831 in C. difficile and heterologously expressing it on the surface of Lactococcus lactis, here we further demonstrated that CD2831 is a collagen-binding protein, able to bind to immobilized collagen types I, III and V as well as native collagen produced by human fibroblasts. We also observed that the overexpression of CD2831 raises the ability to form biofilm on abiotic surface in both C. difficile and L. lactis. Notably, we showed that CD2831 binds to the collagen-like domain of the human complement component C1q, suggesting a role in preventing complement cascade activation via the classical pathway. This functional characterization places CD2831 in the Microbial Surface Components Recognizing Adhesive Matrix Molecule (MSCRAMMs) family, a class of virulence factors with a dual role in adhesion to collagen-rich tissues and in host immune evasion by binding to human complement components.
机译:Clostridium艰难术是革兰氏阳性,厌氧细菌和抗生素相关腹泻和假膜状结肠炎的主要原因。 C.艰难岩通过通过环状偶核苷醇单磷酸(C-DI-GMP)调节的核糖开关的机制来调节其从动机的过渡到无骨骼生活方式。以前描述为由C-DI-GMP阳性调节的分子序列,预测CD2831是胶原蛋白结合蛋白,因此可能参与疗效。通过过度表达CD2831在C.艰难粘附和异源地表达它在乳乳球菌乳酸的表面上,我们进一步证明了CD2831是胶原结合蛋白,能够结合固定的胶原蛋白I,III和V以及由此产生的天然胶原蛋白人的成纤维细胞。我们还观察到CD2831的过表达引发了在C.艰难岩和L.乳酸中的非生物表面形成生物膜的能力。值得注意的是,我们表明CD2831与人补体组分C1Q的胶原样结构域结合,表明通过经典途径预防补体级联激活的作用。这种功能表征将CD2831放置在识别粘合剂基质分子(MSCRAMMS)家族中的CD2831,一类具有双重作用的毒力因子,在富含胶原蛋白的组织和宿主免疫逃逸中具有双重作用,通过与人的补体组分结合。

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