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A synthetic peptide induces long-term protection from lethal infection with herpes simplex virus 2

机译:合成肽可诱导长期保护,防止单纯疱疹病毒2致死性感染

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摘要

Immunization against viral pathogens is generally directed toward the induction of virus neutralizing antibody (VNA) and the maintenance of the potential for a second-set (IgG) response. Indeed, an elevated level of specific antibody is considered a reliable clinical indicator that a state of immunity exists in the host. However, in the case of herpes simplex virus (HSV), the presence of circulating VNA does not necessarily correlate with protection. Thus, it has been found that secondary infections occur in individuals even with high neutralizing titers to HSV, suggesting that antibody to the virus may be useless or even deleterious. In consideration of these facts, we were interested in inducing a T cell response to HSV. We had already shown that synthetic peptides corresponding to the NH3-terminal region of the glycoprotein D (gD) molecule of HSV could induce a strong T cell response when injected into mice, but did not, by themselves, confer protection. In this report, we examined the ability of peptides, covalently coupled to palmitic acid and incorporated into liposomes, to induce virus-specific T cell responses that confer protection against a lethal challenge of HSV-2. We have demonstrated that long-term protective immunity is achieved with a single immunization in the absence of neutralizing antibody when antigen is presented in this form. Furthermore, T cells but not serum from such immune mice can adoptively transfer this protection.
机译:针对病毒病原体的免疫通常是针对病毒中和抗体(VNA)的诱导和第二组(IgG)反应潜力的维持。实际上,特异性抗体水平升高被认为是宿主体内存在免疫状态的可靠临床指标。但是,就单纯疱疹病毒(HSV)而言,循环中的VNA的存在并不一定与保护相关。因此,已经发现即使在中和HSV效价高的情况下,个体仍会发生继发感染,这表明针对该病毒的抗体可能是无用的,甚至是有害的。考虑到这些事实,我们对诱导T细胞对HSV的应答感兴趣。我们已经表明,与HSV糖蛋白D(gD)分子的NH3末端区域相对应的合成肽在注射入小鼠体内后可诱导强烈的T细胞应答,但不能单独提供保护。在本报告中,我们研究了与棕榈酸共价偶联并掺入脂质体的肽诱导病毒特异性T细胞应答的能力,这些应答可赋予针对HSV-2致命性攻击的保护。我们已经证明,当抗原以这种形式存在时,在不存在中和抗体的情况下,单次免疫即可实现长期保护性免疫。而且,来自这种免疫小鼠的T细胞而不是血清可以过继地转移这种保护。

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