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首页> 外文期刊>Developmental Immunology: Journal of Immunology Research >Contribution of the Infection-Associated Complement Regulator-Acquiring Surface Protein 4 (ErpC) to Complement Resistance ofBorrelia burgdorferi
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Contribution of the Infection-Associated Complement Regulator-Acquiring Surface Protein 4 (ErpC) to Complement Resistance ofBorrelia burgdorferi

机译:感染相关补体调节剂获取表面蛋白4(ErpC)对Borrelia burgdorferi补体抗性的贡献。

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Borrelia burgdorferievades complement-mediated killing by interacting with complement regulators through distinct complement regulator-acquiring surface proteins (CRASPs). Here, we extend our analyses to the contribution of CRASP-4 in mediating complement resistance ofB. burgdorferiand its interaction with human complement regulators. CRASP-4 (also known as ErpC) was immobilized onto magnetic beads and used to capture proteins from human serum. Following Western blotting, factor H (CFH), CFH-related protein 1 (CFHR1), CFHR2, and CFHR5 were identified as ligands of CRASP-4. To analyze the impact of native CRASP-4 on mediating survival of serum-sensitive cells in human serum, aB. gariniistrain was generated that ectopically expresses CRASP-4. CRASP-4-producing bacteria bound CFHR1, CFHR2, and CFHR5 but not CFH. In addition, transformed spirochetes deposited significant amounts of lethal complement components on their surface and were susceptible to human serum, thus indicating that CRASP-4 plays a subordinate role in complement resistance ofB. burgdorferi.
机译:伯氏疏螺旋体通过独特的获取补体调节剂的表面蛋白(CRASP)与补体调节剂相互作用,从而实现补体介导的杀伤作用。在这里,我们将分析扩展到CRASP-4在介导B的补体抗性中的作用。 burgdorferi及其与人类补体调节剂的相互作用。 CRASP-4(也称为ErpC)被固定在磁珠上,并用于从人血清中捕获蛋白质。 Western印迹后,因子H(CFH),CFH相关蛋白1(CFHR1),CFHR2和CFHR5被鉴定为CRASP-4的配体。分析天然CRASP-4对介导人血清中血清敏感细胞aB存活的影响。生成了异位表达CRASP-4的gariniistrain。产生CRASP-4的细菌结合CFHR1,CFHR2和CFHR5,但不结合CFH。另外,转化的螺旋体在其表面上沉积大量致死的补体成分,并且对人血清敏感,因此表明CRASP-4在B的补体抗性中起次要作用。伯格多菲里。

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