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编码口蹄疫病毒VP1表位的质粒在小鼠和猪体内引发免疫反应,并保护猪免受病毒感染。

Plasmids encoding foot-and-mouth disease virus VP1 epitopes elicited immune responses in mice and swine and protected swine against viral infection.

作者信息

Wong H T, Cheng S C, Chan E W, Sheng Z T, Yan W Y, Zheng Z X, Xie Y

机构信息

Department of Biology, The Hong Kong University of Science and Technology, Clear Water Bay, Kowloon, China.

出版信息

Virology. 2000 Dec 5;278(1):27-35. doi: 10.1006/viro.2000.0607.

Abstract

VP1 is a capsid protein of foot-and-mouth disease virus (FMDV) and contains epitopes of the virus. Plasmids encoding two VP1 epitopes (amino acid residues 141-160 and 200-213) and a host-self immunoglobulin molecule were constructed to produce a new type of FMD DNA vaccine. Two plasmids, namely, pCEIM and pCEIS, containing mouse immunoglobulin (IgG) or swine IgG were subjected to immunogenicity testing in mice and swine, respectively. In mice administrated pCEIM in the abdomen using a genegun, both FMDV-specific T-cell proliferation and neutralizing antibodies were detected. In swine immunized with pCEIS at the back of the ear, immune responses were achieved after the second administration. Swine showed a T-cell proliferative response with a stimulation index (SI) of up to 8.1 and a neutralizing antibody response that was able to protect suckling mice from 10(2) LD(50) (lethal dose 50) FMDV challenge. To compare the immunogenicity of the DNA-based vaccine candidate, versus the protein-based vaccine candidates, a second group of swine was immunized with the protein F1-scIgG, which was encoded by the plasmid pCEIS. Injection with F1-scIgG elicited a T-cell proliferative response of SI < 1.7 and a neutralizing antibody response that protected suckling mice from up to 10(5) LD(50) FMDV challenge. In the challenge test, three of three swine immunized with pCEIS were fully protected from FMDV challenge.

摘要

VP1是口蹄疫病毒(FMDV)的一种衣壳蛋白,含有该病毒的表位。构建了编码两个VP1表位(氨基酸残基141 - 160和200 - 213)以及一个宿主自身免疫球蛋白分子的质粒,以生产一种新型的口蹄疫DNA疫苗。分别构建了含有小鼠免疫球蛋白(IgG)或猪IgG的两个质粒,即pCEIM和pCEIS,并分别在小鼠和猪中进行免疫原性测试。在用基因枪将pCEIM注射到小鼠腹部后,检测到了口蹄疫病毒特异性T细胞增殖和中和抗体。在用pCEIS免疫猪耳后,第二次给药后产生了免疫反应。猪表现出T细胞增殖反应,刺激指数(SI)高达8.1,并且产生了能够保护乳鼠免受10²半数致死剂量(LD₅₀)口蹄疫病毒攻击的中和抗体反应。为了比较基于DNA的候选疫苗与基于蛋白质的候选疫苗的免疫原性,第二组猪用由质粒pCEIS编码的蛋白质F1 - scIgG进行免疫。注射F1 - scIgG引发了SI < 1.7的T细胞增殖反应以及能够保护乳鼠免受高达10⁵ LD₅₀口蹄疫病毒攻击的中和抗体反应。在攻毒试验中,用pCEIS免疫的三头猪全部受到保护,免受口蹄疫病毒攻击。

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