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Induction of single and dual cytotoxic T-lymphocyte responses to viral proteins in mice using recombinant hybrid Ty-virus-like particles.

机译:使用重组杂合的Ty-病毒样颗粒诱导小鼠对病毒蛋白的单细胞毒和双细胞毒T淋巴细胞反应。

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摘要

The induction of cytotoxic T-lymphocyte (CTL) responses to viral proteins is thought to be an essential component of protective immunity against viral infections. Methods for generating such responses in a reproducible manner would be of great value in vaccine development. We demonstrate here that the recombinant antigen-presentation system based on the yeast transposon (Ty) particle-forming p1 protein is a potent means of inducing CTL responses to a variety of viral CTL epitopes, including influenza virus nucleoprotein (two epitopes), Sendai virus and vesicular stomatitis virus nucleoproteins, and the V3 loop of human immunodeficiency virus type-1 (HIV-1) gp120. CTL were primed by hybrid Ty-virus-like particles (VLP) carrying the minimal epitope or as much as 19,000 MW of protein. Ty-VLP carrying two different epitopes (dual-epitope Ty-VLP) were capable of priming CTL responses in two different strains of mice or against two epitopes in the same individual. Furthermore, co-administration of a mixture of two different Ty-VLP carrying single epitopes could induce responses to both epitopes in the same individual. Ty-VLP appear to represent a reproducible and flexible system for inducing CTL responses in mice, and warrant further evaluation in primates.
机译:诱导对病毒蛋白的细胞毒性T淋巴细胞(CTL)反应被认为是针对病毒感染的保护性免疫的重要组成部分。以可再现的方式产生这种反应的方法在疫苗开发中将具有很大的价值。我们在此证明,基于酵母转座子(Ty)颗粒形成p1蛋白的重组抗原呈递系统是诱导对多种病毒CTL表位包括流感病毒核蛋白(两个表位),仙台病毒的CTL反应的有效手段和水泡性口炎病毒核蛋白,以及人类免疫缺陷病毒1型(HIV-1)gp120的V3环。 CTL由携带最小表位或高达19,000 MW蛋白质的杂交Ty病毒样颗粒(VLP)引发。携带两个不同表位的Ty-VLP(双表位Ty-VLP)能够引发两种不同小鼠品系中的CTL反应或针对同一个体中的两个表位。此外,携带单个表位的两种不同Ty-VLP混合物的共同给药可在同一个体中诱导对两种表位的反应。 Ty-VLP似乎代表了一种可诱导小鼠中CTL反应的可复制且灵活的系统,并需要在灵长类动物中进行进一步评估。

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