编码HIV-1 gp120 +/- IL-15的重组SV40载体诱导对gp120的持久细胞毒免疫应答

Hayley J McKee, Patricia Y T'sao, Maria Vera, Puri Fortes, David S Strayer
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引用次数: 11

摘要

背景:一种能够产生持久、强大的抗hiv免疫的疫苗仍然是一个难以实现的目标。在这些研究中,我们测试了使用病毒载体传递的HIV包膜抗原(gp120)进行多种治疗,无论是否使用IL-15,是否有助于实现这一目标。为此,我们使用了重组标记删除sv40衍生载体(rsv40),因为它们不会引起中和抗体反应,因此可以在不损失转导效率的情况下进行繁殖。方法:SV(gp120)携带HIV-1NL4-3 Env编码序列,SV(mIL-15)携带小鼠IL-15 cDNA。这两种载体分别或联合每月给予BALB/cJ小鼠。使用未选择的效应细胞进行直接细胞毒性试验,检测细胞毒性免疫和细胞毒性记忆。抗体对gp120通过结合试验测定。在这两种情况下,靶细胞都是稳定转染gp120的P815细胞。结果:多次注射SV(gp120)可使未选择的脾细胞产生强大的抗gp120细胞溶解活性(>70%特异性溶解)。多次免疫小鼠的细胞在最后一次注射后休息1年,仍然显示>60%的gp120特异性裂解。注射SV 2个月后首次检测到抗gp120抗体(gp120),此后保持升高。在免疫方案中加入SV(mIL-15)可显著加速记忆细胞溶解反应的发展,两次治疗后1个月特异性溶解>/= 50%。IL-15不改变抗体反应的发展。结论:因此,编码抗原和免疫刺激细胞因子的rSV40s可能是启动和/或增强针对HIV的免疫应答的有用工具。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Durable cytotoxic immune responses against gp120 elicited by recombinant SV40 vectors encoding HIV-1 gp120 +/- IL-15.

BACKGROUND: A vaccine that elicits durable, powerful anti-HIV immunity remains an elusive goal. In these studies we tested whether multiple treatments with viral vector-delivered HIV envelope antigen (gp120), with and without IL-15, could help to approach that goal. For this purpose, we used recombinant Tag-deleted SV40-derived vectors (rSV40s), since they do not elicit neutralizing antibody responses, and so can be given multiply without loss of transduction efficiency. METHODS: SV(gp120) carried the coding sequences for HIV-1NL4-3 Env, and SV(mIL-15) carried the cDNA for mouse IL-15. Singly, and in combination, these two vectors were given monthly to BALB/cJ mice. Cytotoxic immunity and cytotoxic memory were tested in direct cytotoxicity assays using unselected effector cells. Antibody vs. gp120 was measured in a binding assay. In both cases, targets were P815 cells that were stably transfected with gp120. RESULTS: Multiple injections of SV(gp120) elicited powerful anti-gp120 cytolytic activity (>70% specific lysis) by unselected spleen cells. Cells from multiply-immunized mice that were rested 1 year after their last injections still showed >60% gp120-specific lysis. Anti-gp120 antibody was first detected after 2 monthly injections of SV(gp120) and remained elevated thereafter. Adding SV(mIL-15) to the immunization regimen dramatically accelerated the development of memory cytolytic responses, with >/= 50% specific lysis seen 1 month after two treatments. IL-15 did not alter the development of antibody responses. CONCLUSIONS: Thus, rSV40s encoding antigens and immunostimulatory cytokines may be useful tools for priming and/or boosting immune responses against HIV.

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