首页> 美国卫生研究院文献>PLoS Clinical Trials >Immunogenicity and Cross Protective Ability of the Central VP2 Amino Acids of Infectious Pancreatic Necrosis Virus in Atlantic Salmon (Salmo salar L.)
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Immunogenicity and Cross Protective Ability of the Central VP2 Amino Acids of Infectious Pancreatic Necrosis Virus in Atlantic Salmon (Salmo salar L.)

机译:大西洋鲑(Salmo salar L.)传染性胰腺坏死病毒中枢VP2氨基酸的免疫原性和交叉保护能力。

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摘要

Infectious pancreatic necrosis virus (IPNV) is a member of the family Birnaviridae that has been linked to high mortalities in juvenile salmonids and postsmolt stages of Atlantic salmon (Salmo salar L.) after transfer to seawater. IPN vaccines have been available for a long time but their efficacy has been variable. The reason for the varying immune response to these vaccines has not well defined and studies on the importance of using vaccine trains homologous to the virulent field strain has not been conclusive. In this study we prepared one vaccine identical to the virulent Norwegian Sp strain NVI-015 (NCBI: 379740) (T217A221T247 of VP2) and three other vaccine strains developed using the same genomic backbone altered by reverse genetics at three residues yielding variants, T217T221T247, P217A221A247, P217T221A247. These 4 strains, differing in these three positions only, were used as inactivated, oil-adjuvanted vaccines while two strains, T217A221T247 and P217T221A247, were used as live vaccines. The results show that these three residues of the VP2 capsid play a key role for immunogenicity of IPNV vaccines. The virulent strain for inactivated vaccines elicited the highest level of virus neutralization (VN) titers and ELISA antibodies. Interestingly, differences in immunogenicity were not reflected in differences in post challenge survival percentages (PCSP) for oil-adjuvanted, inactivated vaccines but clearly so for live vaccines (TAT and PTA). Further post challenge viral carrier state correlated inversely with VN titers at challenge for inactivated vaccines and prevalence of pathology in target organs inversely correlated with protection for live vaccines. Overall, our findings show that a few residues localized on the VP2-capsid are important for immunogenicity of IPNV vaccines.
机译:传染性胰腺坏死病毒(IPNV)是Birnaviridae家族的一员,该家族与转移到海水中后的幼鲑鱼和大西洋鲑(Salmo salar L.)的蜕皮后阶段的高死亡率有关。 IPN疫苗已经使用很长时间了,但是其功效却是可变的。对这些疫苗产生不同免疫反应的原因尚未明确,关于使用与强毒株同源的疫苗链的重要性的研究尚未得出结论。在这项研究中,我们制备了一种与强毒的挪威Sp毒株NVI-015(NCBI:379740)(VP2的T217A221T247)相同的疫苗,以及使用相同基因组骨架开发的其他三株疫苗株,这些基因组骨架通过反向遗传学在三个残基处产生了变异,即T217T221T247, P217A221A247,P217T221A247。仅在这三个位置不同的这4株菌株被用作灭活的油佐剂疫苗,而T217A221T247和P217T 221 A 247 两种菌株被用作活疫苗。 。结果表明,VP2衣壳的这三个残基对IPNV疫苗的免疫原性起关键作用。灭活疫苗的强毒株引起最高水平的病毒中和(VN)效价和ELISA抗体。有趣的是,免疫原性的差异并未反映在含油佐剂,灭活疫苗的攻击后存活率(PCSP)中,但在活疫苗(TAT和PTA)中则明显。激发后病毒载体的进一步状态与灭活疫苗激发时的VN滴度成反比,而靶器官中病理学的发生率与活疫苗的保护成反比。总体而言,我们的发现表明,位于VP2衣壳上的一些残基对于IPNV疫苗的免疫原性很重要。

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