Earnhart Christopher G, Buckles Eric L, Marconi Richard T
Department of Microbiology and Immunology, Medical College of Virginia at Virginia Commonwealth University, Richmond, VA 23298-0678, USA.
Vaccine. 2007 Jan 5;25(3):466-80. doi: 10.1016/j.vaccine.2006.07.052. Epub 2006 Aug 8.
Lyme disease is the most common arthropod-borne disease in North America and Europe. At present, there is no commercially available vaccine for use in humans. Outer surface protein C (OspC) has antigenic and expression characteristics that make it an attractive vaccine candidate; however, sequence heterogeneity has impeded its use as a vaccinogen. Sequence analyses have identified 21 well defined OspC phyletic groups or "types" (designated A-U). In this report we have mapped the linear epitopes presented by OspC types B, K, and D during human and murine infection and exploited these epitopes (along with the previously identified type A OspC linear epitopes) in the development of a recombinant, tetravalent, chimeric vaccinogen. The construct was found to be highly immunogenic in mice and the induced antibodies surface labeled in vitro cultivated spirochetes. Importantly, vaccination induced complement-dependent bactericidal antibodies against strains expressing each of the OspC types that were incorporated into the construct. These results suggest that an effective and broadly protective polyvalent OspC-based Lyme disease vaccine can be produced as a recombinant, chimeric protein.
莱姆病是北美和欧洲最常见的节肢动物传播疾病。目前,尚无用于人类的商业化疫苗。外表面蛋白C(OspC)具有抗原性和表达特性,使其成为有吸引力的疫苗候选物;然而,序列异质性阻碍了其作为疫苗原的使用。序列分析已确定21个明确的OspC系统发育组或“类型”(命名为A - U)。在本报告中,我们绘制了人类和小鼠感染期间OspC B型、K型和D型呈现的线性表位,并在重组四价嵌合疫苗原的开发中利用了这些表位(以及先前鉴定的A型OspC线性表位)。该构建体在小鼠中具有高度免疫原性,诱导的抗体可在体外培养的螺旋体上进行表面标记。重要的是,接种疫苗诱导了针对表达构建体中包含的每种OspC类型菌株的补体依赖性杀菌抗体。这些结果表明,可以生产一种有效的、具有广泛保护作用的基于多价OspC的莱姆病重组嵌合蛋白疫苗。
