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Virulence-associated trimeric autotransporters of Haemophilus parasuis are antigenic proteins expressed in vivo

机译:副猪嗜血杆菌的毒力相关三聚体自转运蛋白是体内表达的抗原蛋白

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摘要

Glässer’s disease is a re-emerging swine disease characterized by a severe septicaemia. Vaccination has been widely used to control the disease, although there is a lack of extended cross-protection. Trimeric autotransporters, a family of surface exposed proteins implicated in host-pathogen interactions, are good vaccine candidates. Members of this family have been described in Haemophilus parasuis and designated as virulence-associated trimeric autotransporters (VtaA). In this work, we produced 15 recombinant VtaA passenger domains and looked for the presence of antibodies directed against them in immune sera by immunoblotting. After infection with a subclinical dose of H. parasuis Nagasaki, an IgG mediated antibody response against 6 (VtaA1, 5, 6, 8, 9 and 10) of the 13 VtaA of the Nagasaki strain was detected, indicating that they are expressed in vivo. IgA production against VtaA was detected in only one animal. VtaA were more likely to be late antigens when compared to early (Omp P5 and Omp P6) and late (YaeT) defined antigens. Antibody cross-reaction with two orthologs of Nagasaki’s VtaA5 and 6, VtaA15 and 16 of strain HP1319, was also detected. No antibodies against VtaA were detected in the sera of animals immunized with a bacterin of the Nagasaki strain, suggesting poor expression in the in vitro conditions used. Taken together, these results indicate that VtaA are good candidate immunogens that could be used to improve H. parasuis vaccines. However, their capacity to confer protective immunity needs to be further studied.
机译:格拉瑟氏病是一种以严重败血病为特征的新出现的猪病。疫苗接种已广泛用于控制该疾病,尽管缺乏扩展的交叉保护作用。三聚体自转运蛋白是一种与宿主-病原体相互作用有关的表面暴露蛋白家族,是很好的候选疫苗。该家族的成员已在副猪嗜血杆菌中描述,并被指定为与毒力相关的三聚体自转运蛋白(VtaA)。在这项工作中,我们产生了15个重组VtaA客体结构域,并通过免疫印迹法寻找在免疫血清中针对它们的抗体的存在。用亚临床剂量的副猪嗜血杆菌长崎感染后,检测到针对长崎菌株13个VtaA中的6个(VtaA1、5、6、8、9和10)的IgG介导的抗体应答,表明它们在体内表达。仅在一只动物中检测到针对VtaA的IgA产生。与早期(Omp P5和Omp P6)和晚期(YaeT)定义的抗原相比,VtaA更可能是晚期抗原。还检测到了与长崎的两个直系同源物HP1319株的VtaA5和6,VtaA15和16的直系同源物的抗体交叉反应。在用长崎菌株的菌苗免疫的动物血清中未检测到针对VtaA的抗体,表明在所用体外条件下表达较差。综上所述,这些结果表明VtaA是可以用于改善副猪嗜血杆菌疫苗的良好候选免疫原。但是,它们赋予保护性免疫的能力有待进一步研究。

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