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The Tat protein broadens T cell responses directed to the HIV-1 antigens Gag and Env: Implications for the design of new vaccination strategies against AIDS

机译:Tat蛋白扩大了针对HIV-1抗原Gag和Env的T细胞反应:对设计新的针对AIDS的疫苗接种策略的意义

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We have previously shown that the biologically active Tat protein targets and efficiently enters dendritic cells, and increases the proteolytic activities of the immunoproteasome, thereby favoring the generation and presentation of the subdominant MHC-I binding CTL epitopes of heterologous antigens. In the present study, we demonstrate that Tat broadens in vivo epitope-specific T cell responses directed to heterologous antigens including HIV structural proteins. Specifically, co-immunization of mice with OVA and Tat proteins induces CTL responses against subdominant and cryptic OVA-derived epitopes, which are not detected in mice vaccinated with OVA alone. Similarly, mice vaccinated with the HIV-1 Gag, Env or V2-deleted Env antigens in combination with Tat show Th1-type and CTL responses directed to a larger number of T cell epitopes, as compared to mice vaccinated with these proteins in absence of Tat. In contrast, Tat did not affect Th2-type responses to these structural HIV proteins. These results indicate that Tat is not only an antigen but also a novel Th1-type adjuvant capable of broadening in vivo the spectrum of epitopes recognized by T cells, and suggest that Tat can be considered an optimal co-antigen in the development of novel vaccination strategies against AIDS.
机译:我们先前已经表明,具有生物活性的Tat蛋白靶向并有效进入树突状细胞,并增加了免疫蛋白酶体的蛋白水解活性,从而有利于异源抗原的主要MHC-1结合CTL表位的产生和呈现。在本研究中,我们证明Tat扩大了针对异源抗原(包括HIV结构蛋白)的体内表位特异性T细胞应答。具体而言,用OVA和Tat蛋白对小鼠进行共免疫可诱导针对主要和隐秘的OVA衍生抗原决定簇的CTL反应,这在单独接种OVA的小鼠中未检测到。类似地,与未接种HIV-1 Gag,Env或V2的Env抗原结合Tat疫苗接种的小鼠相比,接种了这些蛋白的小鼠显示出针对大量T细胞表位的Th1型和CTL反应。达相反,Tat不会影响Th2型对这些结构性HIV蛋白的反应。这些结果表明,Tat不仅是一种抗原,而且还是一种新型的Th1型佐剂,能够在体内拓宽T细胞识别的抗原决定簇的范围,并表明Tat可以被认为是新型疫苗开发中的最佳协同抗原。艾滋病防治策略。

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