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重组二聚体小免疫蛋白在体外能有效中和传染性胃肠炎病毒的感染性,并在体内赋予被动免疫力。

Recombinant dimeric small immunoproteins neutralize transmissible gastroenteritis virus infectivity efficiently in vitro and confer passive immunity in vivo.

作者信息

Bestagno Marco, Sola Isabel, Dallegno Eliana, Sabella Patricia, Poggianella Monica, Plana-Durán Juan, Enjuanes Luis, Burrone Oscar R

机构信息

International Centre for Genetic Engineering and Biotechnology, AREA Science Park, Padriciano 99, 34012 Trieste, Italy.

Department of Molecular and Cell Biology, Centro Nacional de Biotecnologia, Consejo Superior de Investigaciones Cientificas, Campus Univ. Autonoma Madrid, Darwin 3, Cantoblanco, 28049 Madrid, Spain.

出版信息

J Gen Virol. 2007 Jan;88(Pt 1):187-195. doi: 10.1099/vir.0.82192-0.

DOI:10.1099/vir.0.82192-0
PMID:17170451
Abstract

Small immunoproteins (SIPs) are single-chain molecules comprising the variable regions of an antibody assembled in a single polypeptide (scFv) and joined to the immunoglobulin heavy-chain dimerizing domain. To investigate the potential of these molecules to provide protection against enteric infections when supplied orally, SIPs were generated against Transmissible gastroenteritis virus (TGEV), a highly pathogenic porcine virus. Different variants of TGEV-specific SIPs were created, of epsilon and alpha isotypes, by exploiting the dimerizing domains epsilonCH4 and alphaCH3 of human and swine origin. Transfected cells secreted these recombinant mini-antibodies efficiently, mainly as dimers stabilized covalently by inter-chain disulphide bridges. The specificity and functionality of the recombinant TGEV-specific SIPs were determined by in vitro binding, neutralization and infection-interference assays. The neutralization indices of the TGEV-specific SIPs were all very similar to that of the original TGEV-specific mAb, thus confirming that the immunological properties have been preserved in the recombinant SIPs. In vivo protection experiments on newborn piglets have, in addition, demonstrated a strong reduction of virus titre in infected tissues of animals treated orally with TGEV-specific SIPs. It has therefore been demonstrated that it is possible to confer passive immunization to newborn pigs by feeding them with recombinant SIPs.

摘要

小型免疫蛋白(SIPs)是单链分子,由组装在一条多肽链中的抗体可变区(scFv)组成,并与免疫球蛋白重链二聚化结构域相连。为了研究这些分子经口服提供针对肠道感染的保护作用的潜力,制备了针对猪传染性胃肠炎病毒(TGEV,一种高致病性猪病毒)的SIPs。通过利用人和猪源的二聚化结构域epsilonCH4和alphaCH3,构建了epsilon和alpha同种型的TGEV特异性SIPs的不同变体。转染细胞高效分泌这些重组微型抗体,主要以通过链间二硫键共价稳定的二聚体形式存在。通过体外结合、中和及感染干扰试验确定重组TGEV特异性SIPs的特异性和功能。TGEV特异性SIPs的中和指数与原始TGEV特异性单克隆抗体的中和指数都非常相似,从而证实重组SIPs保留了免疫特性。此外,对新生仔猪的体内保护实验表明,用TGEV特异性SIPs口服处理的动物感染组织中的病毒滴度大幅降低。因此已经证明,通过给新生仔猪喂食重组SIPs可以使其获得被动免疫。

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