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牛流行热病毒糖蛋白G基因的DNA序列分析及牛流行热双油乳剂疫苗的研制

DNA sequence analysis of glycoprotein G gene of bovine ephemeral fever virus and development of a double oil emulsion vaccine against bovine ephemeral fever.

作者信息

Hsieh Yao-Ching, Wang Shiang-Yiu, Lee Yen-Feng, Chen Shih-Hui, Mak Paul O T, Chu Chun-Yen

机构信息

Graduate Institute of Animal Vaccine Technology, National Pingtung University of Science and Technology No.1, Taiwan.

出版信息

J Vet Med Sci. 2006 Jun;68(6):543-8. doi: 10.1292/jvms.68.543.

Abstract

The surface glycoprotein G is considered as the major neutralizing and protective antigen of bovine ephemeral fever virus (BEFV). Comparison of the deduced amino acid sequence of G protein of BEFV isolates during the period 1984-2004 outbreaks in Taiwan showed amino acid substitutions in the neutralizing epitopes. All the isolates differ markedly in the neutralizing epitope at the same amino acid positions compared to the currently available killed vaccine strain (Tn73). Tn88128 strain isolated in 1999 showed the maximum variability of 12 amino acids, 5 amino acid in the neutralization epitope and 7 apart from, respectively. Combinations of both Tn88128 (1999) and commercially available vaccine strain (Tn73) were developed and its safety was evaluated in mice, guinea pigs, calves, and pregnant cows. None of the animals showed any adverse effect or clinical signs. Calves were immunized with commercial vaccine (Tn73) and, combined vaccine (Tn73 and Tn88128), respectively, with adjuvants such as Al-gel and water-in-oil-in-water (w/o/w) oil and PBS alone and challenged with Tn88128 strains. Except PBS administered animals, all the vaccinated animals showed protective immune response. However, animals immunized with combined vaccine plus w/o/w adjuvant elicited stronger neutralization antibodies and long lasting immunity compared to other vaccines.

摘要

表面糖蛋白G被认为是牛暂时热病毒(BEFV)的主要中和及保护性抗原。对1984 - 2004年台湾地区疫情期间BEFV分离株G蛋白推导氨基酸序列的比较显示,中和表位存在氨基酸替换。与目前可用的灭活疫苗株(Tn73)相比,所有分离株在相同氨基酸位置的中和表位上均有显著差异。1999年分离的Tn88128株显示出最大变异性,有12个氨基酸变异,其中5个在中和表位,7个在其他位置。开发了Tn88128(1999)与市售疫苗株(Tn73)的组合,并在小鼠、豚鼠、犊牛和怀孕母牛中评估了其安全性。所有动物均未出现任何不良反应或临床症状。分别用商业疫苗(Tn73)、联合疫苗(Tn73和Tn88128)加佐剂(如铝胶、水包油包水(w/o/w)油)和单独的PBS对犊牛进行免疫,并用Tn88128株进行攻毒。除了给予PBS的动物外,所有接种疫苗的动物均表现出保护性免疫反应。然而,与其他疫苗相比,用联合疫苗加w/o/w佐剂免疫的动物产生更强的中和抗体和持久免疫力。

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