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首页> 外文期刊>Maydica >Dendritic cell-targeted porcine reproductive and respiratory syndrome virus (PRRSV) antigens adjuvanted with polyinosinic-polycytidylic acid (poly (I:C)) induced non-protective immune responses against heterologous type 2 PRRSV challenge in pigs
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Dendritic cell-targeted porcine reproductive and respiratory syndrome virus (PRRSV) antigens adjuvanted with polyinosinic-polycytidylic acid (poly (I:C)) induced non-protective immune responses against heterologous type 2 PRRSV challenge in pigs

机译:用多胞聚环酸(Poly(I:C))诱导对猪的异源2型PRRSV攻击的非保护免疫反应诱导非保护免疫应答的树突状细胞靶向猪生殖和呼吸综合征病毒(PRRSV)抗原

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Porcine Reproductive and Respiratory Syndrome (PRRS) is an economically important swine viral disease worldwide. Current modified live-attenuated vaccines are ineffective against heterologous strains of PRRS virus (PRRSV) circulating in the field. In this study, we evaluated three dendritic cell (DC)-targeted vaccine candidates for their protective efficacy against heterologous PRRSV challenge. Ectodomain regions of DNA-shuffled structural proteins GP3, GP4, GP5 and M of PRRSV were fused together to form the vaccine antigen which was in turn fused with one of three recombinant antibodies each specific to a DC receptor: DC-SIGN, Langerin, and DEC205. The recombinant antibody-fused vaccine antigens were co-administered with polyinosinic-polycytidylic acid (poly (I:C)) adjuvant and subsequently challenged with a heterologous type 2 PRRSV strain (NADC20) in pigs. Our results demonstrate that pigs in DC-SIGN- and DEC205-targeted, but not Langerin- and non-targeted, vaccine groups showed significant IFN-gamma- and IL-4-specific CD4T cell immune responses against the vaccine antigen in 7 days post-challenge. Pigs in DC-SIGN- and Langerin-targeted vaccine groups showed greatly reduced IgG responses as compared to the DEC205- and non-targeted vaccine groups. The immune responses induced by DC-targeted vaccines did not reduce viremia and lung pathological lesions in type 2 PRRSV-challenged pigs. In contrast, pigs in Langerin-targeted vaccine group showed significantly increased serum viral titers and viral antigen in lung tissues at 7 and 14 days post-challenge respectively. In conclusion, specific targeting of PRRSV antigen through DC-SIGN or DEC205 or Langerin-specific antibodies in the presence of poly (I:C) adjuvant induced immune responses that failed to protect pigs against heterologous type 2 PRRSV challenge.
机译:猪繁殖和呼吸综合征(PRRS)是全球经济上重要的猪病毒疾病。目前改性的活衰减疫苗对现场循环的PRRS病毒(PRRSV)的异源菌株无效。在这项研究中,我们评估了三种树突细胞(DC)的疫苗候选候选候选患者免受异源PRRSV挑战的保护效果。 PRRSV的DNA淋上结构蛋白GP3,GP4,GP5和M的外域区域融合在一起以形成疫苗抗原,其依次与三种重组抗体中的一种融合,每种重组抗体中的一种,每种特定于DC受体:DC-SIGN,LANGERIN和DEC205。将重组抗体熔融疫苗抗原与多胞菌 - 多环酸(聚(I:C))佐剂共同施用,随后用猪中的异源型2 PRRSV菌株(NADC20)攻击。我们的结果表明,DC标志和DEC205靶向的猪和非靶向植物和非靶向的疫苗基团在7天柱中显示出对疫苗抗原的显着的IFN-Gamma-和IL-4特异性CD4T细胞免疫反应-挑战。与DEC205-和非靶向疫苗组相比,DC-SIGN和LANGERIN靶向疫苗基团中的猪表现出极大地降低IgG响应。 DC靶向疫苗诱导的免疫应答未降低2型PRRSV攻击性猪中的病毒血症和肺病理病变。相比之下,在攻击后7和14天的肺组织中患有显着增加的血清病毒滴度和病毒抗原显着增加了血清病毒滴度和病毒抗原。总之,通过DC-SIGN或DEC205或Langerin特异性抗体在Poly(I:C)佐剂诱导的免疫反应存在下进行PRRSV抗原的特异性靶向,所述免疫应答未能保护猪免受异源2型PRRSV攻击。

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