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确定杜克雷嗜血杆菌三聚体自转运黏附素DsrA的潜在疫苗靶点

Defining Potential Vaccine Targets of Haemophilus ducreyi Trimeric Autotransporter Adhesin DsrA.

作者信息

Fusco William G, Choudhary Neelima R, Stewart Shelley M, Alam S Munir, Sempowski Gregory D, Elkins Christopher, Leduc Isabelle

机构信息

1 Department of Medicine, University of North Carolina at Chapel Hill , North Carolina.

出版信息

Monoclon Antib Immunodiagn Immunother. 2015 Apr;34(2):73-82. doi: 10.1089/mab.2014.0054.

Abstract

Haemophilus ducreyi is the causative agent of the sexually transmitted genital ulcer disease chancroid. Strains of H. ducreyi are grouped in two classes (I and II) based on genotypic and phenotypic differences, including those found in DsrA, an outer membrane protein belonging to the family of multifunctional trimeric autotransporter adhesins. DsrA is a key serum resistance factor of H. ducreyi that prevents binding of natural IgM at the bacterial surface and functions as an adhesin to fibronectin, fibrinogen, vitronectin, and human keratinocytes. Monoclonal antibodies (MAbs) were developed to recombinant DsrA (DsrA(I)) from prototypical class I strain 35000HP to define targets for vaccine and/or therapeutics. Two anti-DsrAI MAbs bound monomers and multimers of DsrA from genital and non-genital/cutaneous H. ducreyi strains in a Western blot and reacted to the surface of the genital strains; however, these MAbs did not recognize denatured or native DsrA from class II strains. In a modified extracellular matrix protein binding assay using viable H. ducreyi, one of the MAbs partially inhibited binding of fibronectin, fibrinogen, and vitronectin to class I H. ducreyi strain 35000HP, suggesting a role for anti-DsrA antibodies in preventing binding of H. ducreyi to extracellular matrix proteins. Standard ELISA and surface plasmon resonance using a peptide library representing full-length, mature DsrAI revealed the smallest nominal epitope bound by one of the MAbs to be MEQNTHNINKLS. Taken together, our findings suggest that this epitope is a potential target for an H. ducreyi vaccine.

摘要

杜克雷嗜血杆菌是性传播的生殖器溃疡性疾病软下疳的病原体。基于基因型和表型差异,杜克雷嗜血杆菌菌株分为两类(I类和II类),这些差异包括在DsrA中发现的差异,DsrA是一种外膜蛋白,属于多功能三聚体自转运黏附素家族。DsrA是杜克雷嗜血杆菌的关键血清抗性因子,可防止天然IgM在细菌表面结合,并作为纤连蛋白、纤维蛋白原、玻连蛋白和人角质形成细胞的黏附素发挥作用。针对来自I类原型菌株35000HP的重组DsrA(DsrA(I))开发了单克隆抗体(MAb),以确定疫苗和/或治疗药物的靶点。两种抗DsrAI单克隆抗体在蛋白质印迹中与来自生殖器和非生殖器/皮肤杜克雷嗜血杆菌菌株的DsrA单体和多聚体结合,并与生殖器菌株表面发生反应;然而,这些单克隆抗体不能识别II类菌株的变性或天然DsrA。在使用活的杜克雷嗜血杆菌的改良细胞外基质蛋白结合试验中,其中一种单克隆抗体部分抑制了纤连蛋白、纤维蛋白原和玻连蛋白与I类杜克雷嗜血杆菌菌株35000HP的结合,表明抗DsrA抗体在防止杜克雷嗜血杆菌与细胞外基质蛋白结合中发挥作用。使用代表全长成熟DsrAI的肽库进行的标准ELISA和表面等离子体共振显示,其中一种单克隆抗体结合的最小标称表位为MEQNTHNINKLS。综上所述,我们的研究结果表明,该表位是杜克雷嗜血杆菌疫苗的潜在靶点。

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