以 RecA 和 FliD 为抗原的异源 DNA 初免-蛋白加强免疫可提供针对钩端螺旋体感染的跨血清型保护。
Heterologous DNA prime-protein boost immunization with RecA and FliD offers cross-clade protection against leptospiral infection.
机构信息
Medical Microbiology Laboratory, Department of Microbiology, Centre of Excellence in Life Sciences, Bharathidasan University, Tiruchirappalli, 620 024, Tamilnadu, India.
Lewis Katz School of Medicine, Temple University, Philadelphia, PA, 19140, USA.
出版信息
Sci Rep. 2018 Apr 24;8(1):6447. doi: 10.1038/s41598-018-24674-8.
The emergence of >300 serovars of Leptospira confounded the use of generalized bacterin, the whole cell lysate, as vaccines to control leptospirosis. Because of substantial genetic and geographic heterogeneity among circulating serovars, one vaccine strain per serovar cannot be efficacious against all the serovars. We have performed heterologous DNA prime-protein boost vaccination challenge studies in hamsters using in vivo expressed, leptospiral recombinase A (RecA) and flagellar hook associated protein (FliD). We prepared the monovalent recombinant protein, plasmid DNA, and DNA prime protein boost adjuvant vaccines. The whole cell bacterin served as a control. Our data show that (i) RecA and FliD have multiple immunogenic B and T-cell epitopes with highly conserved domains among most prevalent pathogenic Leptospira spp., (ii) humoral and cell mediated immune responses were induced remarkably, (iii) provides significant protection against homologous (Autumnalis strain N2) and cross-clade heterologous (Canicola strain PAI-1) challenge infection for the heterologous prime-protein boost (∼91-100%) and, the DNA vaccine (∼75-83%). Recombinant protein vaccine shows only partial protection (∼58-66%), (iv) RecA prime-protein boost vaccine shows sterilizing immunity, with heterologous protection. This RecA/FliD prime-protein boost strategy holds potential for vaccination against animal leptospirosis and for a better control of zoonotic transmission.
超过 300 种钩端螺旋体血清型的出现使得使用通用疫苗,即全细胞裂解物作为疫苗来控制钩端螺旋体病变得复杂。由于循环血清型之间存在大量的遗传和地理异质性,因此每一种血清型都不能使用一种疫苗来有效对抗所有血清型。我们使用体内表达的重组酶 A (RecA) 和鞭毛钩相关蛋白 (FliD) 在仓鼠中进行了异源 DNA 初免-蛋白加强接种挑战研究。我们制备了单价重组蛋白、质粒 DNA 和 DNA 初免-蛋白加强佐剂疫苗。全细胞菌苗作为对照。我们的数据表明:(i) RecA 和 FliD 具有多个免疫原性 B 和 T 细胞表位,在大多数流行的致病性钩端螺旋体属中具有高度保守的结构域;(ii) 体液和细胞介导的免疫反应显著增强;(iii) 对同源 (Autumnalis 株 N2) 和交叉谱系异源 (Canicola 株 PAI-1) 挑战感染提供了显著的保护作用,异源初免-蛋白加强 (约 91-100%) 和 DNA 疫苗 (约 75-83%);重组蛋白疫苗仅提供部分保护 (约 58-66%);(iv) RecA 初免-蛋白加强疫苗显示出杀菌性免疫,具有异源保护作用。这种 RecA/FliD 初免-蛋白加强策略具有针对动物钩端螺旋体病的疫苗接种潜力,并可更好地控制人畜共患病传播。
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