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Activation of HIV-1-specific immune responses to an HIV-1 vaccine constructed from a replication-defective adenovirus vector using various combinations of immunization protocols

机译:使用多种免疫方案组合激活从复制缺陷型腺病毒载体构建的HIV-1疫苗对HIV-1特异性免疫反应

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摘要

We constructed a recombinant replication defective adenovirus vector containing the env gene (Ad-Bal) derived from macrophage-trophic HIV-1 (HIV-1 Bal). We then immunized mice with this vector using several administration routes and protocols, and examined the immune response. When the Ad-Bal viral vector (over 1 × 107 pfu) was injected subcutaneously, both humoral and cell-mediated immunities were induced. However, immune response induced by the Ad-Bal vector alone was weaker than that induced by the recombinant vaccinia viral vector. We then employed the following three immunization protocols: (l) DNA vaccination followed by immunization with the Ad-Bal; (2) vaccination using the Ad-Bal vector followed by DNA vaccination; and (3) DNA vaccination followed by Ad-Bal infection and passive transfer of dendritic cells (DCs) infected with the Ad-Bal. Among the three protocols, the last gave the strongest humoral and cell-mediated immunity. These results suggest that the combination of DNA vaccination, Ad-Bal vector infection and passive transfer of Ad-Bal-infected DCs can induce strong immunity against HIV-1 Bal.
机译:我们构建了一个重组复制缺陷型腺病毒载体,其中包含衍生自巨噬细胞营养性HIV-1(HIV-1 Bal)的env基因(Ad-Bal)。然后,我们使用几种给药途径和方案将此载体免疫小鼠,并检查了免疫应答。皮下注射Ad-Bal病毒载体(超过1×107 pfu)时,可诱导体液免疫和细胞介导的免疫。然而,仅由Ad-Bal载体诱导的免疫应答比由重组痘苗病毒载体诱导的免疫应答弱。然后,我们采用以下三种免疫方案:(1)DNA疫苗接种,然后用Ad-Bal免疫; (2)使用Ad-Bal载体进行疫苗接种,然后进行DNA疫苗接种; (3)接种DNA疫苗,然后进行Ad-Bal感染,然后被动转移感染Ad-Bal的树突状细胞(DC)。在这三个方案中,最后一个方案具有最强的体液和细胞介导的免疫力。这些结果表明,DNA疫苗接种,Ad-Bal载体感染和Ad-Bal感染的DC的被动转移的结合可以诱导针对HIV-1 Bal的强大免疫力。

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