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牛病毒性腹泻病毒疫苗的免疫学

Immunology of BVDV vaccines.

作者信息

Ridpath Julia F

机构信息

Ruminant Diseases and Immunology Research Unit, National Animal Disease Center, ARS/USDA, PO Box 70, 1920 Dayton Avenue, Ames, IA 50010, USA.

出版信息

Biologicals. 2013 Jan;41(1):14-9. doi: 10.1016/j.biologicals.2012.07.003. Epub 2012 Aug 9.

Abstract

Providing acquired immune protection against infection with bovine viral diarrhea viruses (BVDV) is challenging due to the heterogeneity that exists among BVDV strains and the ability of the virus to infect the fetus and establish persistent infections. Both modified live and killed vaccines have been shown to be efficacious under controlled conditions. Both humoral and cellular immune responses are protective. Following natural infection or vaccination with a modified live vaccine, the majority of the B cell response (as measured by serum antibodies) is directed against the viral proteins E2 and NS2/3, with minor responses against the Erns and E1 proteins. Vaccination with killed vaccines results in serum antibodies directed mainly at the E2 protein. It appears that the major neutralizing epitopes are conformational and are located within the N-terminal half of the E2 protein. While it is thought that the E2 and NS2/3 proteins induce protective T cell responses, these epitopes have not been mapped. Prevention of fetal infections requires T and B cell response levels that approach sterilizing immunity. The heterogeneity that exists among circulating BVDV strains, works against establishing such immunity. Vaccination, while not 100% effective in every individual animal, is effective at the herd level.

摘要

由于牛病毒性腹泻病毒(BVDV)毒株之间存在异质性,且该病毒能够感染胎儿并建立持续性感染,因此提供针对BVDV感染的获得性免疫保护具有挑战性。在可控条件下,减毒活疫苗和灭活疫苗均已证明有效。体液免疫和细胞免疫反应均具有保护作用。在自然感染或接种减毒活疫苗后,大多数B细胞反应(通过血清抗体检测)针对病毒蛋白E2和NS2/3,对Erns和E1蛋白的反应较弱。接种灭活疫苗会产生主要针对E2蛋白的血清抗体。主要的中和表位似乎是构象性的,位于E2蛋白的N端一半区域内。虽然认为E2和NS2/3蛋白可诱导保护性T细胞反应,但这些表位尚未定位。预防胎儿感染需要接近无菌免疫的T细胞和B细胞反应水平。循环BVDV毒株之间存在的异质性不利于建立这种免疫。疫苗接种虽然并非对每只动物都100%有效,但在畜群水平上是有效的。

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