该类毒素作为血清阴性受试者预防性疫苗的组成部分。

A Gringeri, E Santagostino, M Muça-Perja, H Le Buanec, B Bizzini, A Lachgar, J F Zagury, J Rappaport, A Burny, R C Gallo, D Zagury
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引用次数: 39

摘要

由于Tat蛋白(一种诱导免疫抑制和细胞凋亡的HIV-1毒素)的施用可能对宿主免疫系统有害,因此使用化学灭活但仍具有免疫原性的Tat制剂Tat类毒素对血清阴性个体进行Tat免疫。在一项公开的、对照的I期临床试验中,Tat类毒素被证明是安全的、耐受性良好的,并且能够引发特定的免疫反应。特别是,在所有5名免疫研究对象中,免疫后观察到针对天然Tat的循环抗体增加了3倍至10倍以上,并且在体内对Tat类毒素的延迟型超敏反应(DTH)皮肤试验中呈阳性反应,体外对天然Tat的淋巴细胞增生性反应增加。持续(>或=1年)高水平的循环抗tat抗体可以防止tat诱导的免疫抑制,并且在HIV-1暴露后,允许抗HIV-1细胞免疫反应,其早期释放保护性β趋化因子,导致宿主抗性增加,即保护。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tat toxoid as a component of a preventive vaccine in seronegative subjects.

Because administration of Tat protein, the HIV-1 toxin that induces immunosuppression and apoptosis, may be deleterious to the host immune system, a chemically inactivated but nonetheless immunogenic Tat preparation, Tat toxoid, was used to immunize seronegative individuals against Tat. In an open, controlled, phase I clinical trial, Tat toxoid turned out to be safe, well tolerated, and able to trigger a specific immune reaction. In particular, a threefold to more than 10-fold increase of circulating antibodies directed against the native Tat was observed after immunization in all of 5 immunized study subjects, together with a positive reaction to delayed-type hypersensitivity (DTH) skin test with Tat toxoid in vivo and increased lymphoproliferative response to native Tat in vitro. Persistent (> or =1 year) high levels of circulating anti-Tat antibodies could prevent the Tat-induced immune suppression and, following HIV-1 exposure, allow the anti-HIV-1 cellular immune response, with its early release of protective beta-chemokines, to occur leading to an increase of host resistance, that is, protection.

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