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首页> 外文期刊>Infection and immunity >The Dominant Epitope of Borrelia garinii Outer Surface Protein C Recognized by Sera from Patients with Neuroborreliosis Has a Surface-Exposed Conserved Structural Motif
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The Dominant Epitope of Borrelia garinii Outer Surface Protein C Recognized by Sera from Patients with Neuroborreliosis Has a Surface-Exposed Conserved Structural Motif

机译:血清神经营养不良患者所识别的疏螺旋体外表面蛋白C的主要表位具有表面暴露的保守结构基序

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Epitope mapping of outer surface protein C (OspC) by using sera from patients with neuroborreliosis led to the identification of one single major immunodominant epitope within the C-terminal 10 amino acid residues. Peptide binding studies and alanine replacement scanning of the C-terminal decapeptide, PVVAESPKKP, revealed a critical role for the PKKP sequence and its terminal carboxyl group for the binding of immunoglobulin M (IgM) antibodies from patients with Lyme borreliosis. Electron microscopy of antibody-labeled spirochetes indicated that the C-terminal region is exposed on the surface of the spirochete. Based on homology to proteins of known function, this region most probably adopts a polyproline II-like helix, which is found in surface-exposed structures involved in protein-protein interactions. This structural motif is highly conserved in Borrelia species causing Lyme borreliosis and subjected to purifying selection. We suggest that the abundance of the C-terminal region of OspC on the surface of B. burgdorferi allows a multimeric high-avidity interaction between the spirochete and surface Igs on B cells. The resulting cross-linking of surface Igs on B cells may induce a T-cell-independent B-cell activation without IgM-to-IgG switching, thus explaining the lack of IgG antibodies to OspC in neuroborreliosis.
机译:通过使用来自神经性贝氏体病患者的血清进行外表面蛋白C(OspC)的表位作图,导致在C端10个氨基酸残基内鉴定出一个单一的主要免疫优势表位。肽结合研究和C末端十肽PVVAESPKKP的丙氨酸替代扫描揭示了PKKP序列及其末端羧基对莱姆病患者的免疫球蛋白M(IgM)抗体结合的关键作用。抗体标记的螺旋体的电子显微镜观察表明,C末端区域暴露在螺旋体的表面上。基于与已知功能蛋白质的同源性,该区域最可能采用多脯氨酸II样螺旋,该螺旋在涉及蛋白质-蛋白质相互作用的表面暴露结构中发现。该结构基序在 Borrelia 物种中高度保守,从而引起莱姆病(Lyme borreliosis),并经过纯化选择。我们建议在 B表面上存在OspC的C末端区域的丰度。 burgdorferi 允许螺旋体与B细胞表面Igs之间发生多聚体高亲和力相互作用。 B细胞上表面Igs的最终交联可能会诱导不依赖T细胞的B细胞活化,而无需IgM到IgG的转换,从而解释了神经性贝氏体病缺乏针对OspC的IgG抗体。

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