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鼻腔和皮肤给药的 IC31(®)-佐剂重组单纯疱疹病毒 2 糖蛋白 D 可预防生殖器疱疹。

Nasal and skin delivery of IC31(®)-adjuvanted recombinant HSV-2 gD protein confers protection against genital herpes.

机构信息

Intercell AG, Campus Vienna Biocenter 3, 1030 Vienna, Austria.

出版信息

Vaccine. 2012 Jun 19;30(29):4361-8. doi: 10.1016/j.vaccine.2012.02.019.

DOI:10.1016/j.vaccine.2012.02.019
PMID:22682292
Abstract

Genital herpes caused by herpes simplex virus type 2 (HSV-2) remains the leading cause of genital ulcers worldwide. Given the disappointing results of the recent genital herpes vaccine trials in humans, development of novel vaccine strategies capable of eliciting protective mucosal and systemic immune responses to HSV-2 is urgently required. Here we tested the ability of the adjuvant IC31(®) in combination with HSV-2 glycoprotein D (gD) used through intranasal (i.n.), intradermal (i.d.), or subcutaneous (s.c.) immunization routes for induction of protective immunity against genital herpes infection in C57BL/6 mice. Immunization with gD plus IC31(®) through all three routes of immunization developed elevated gD-specific serum antibody responses with HSV-2 neutralizing activity. Whereas the skin routes promoted the induction of a mixed IgG2c/IgG1 isotype profile, the i.n. route only elicited IgG1 antibodies. All immunization routes were able to induce gD-specific IgG antibody responses in the vaginas of mice immunized with IC31(®)-adjuvanted gD. Although specific lymphoproliferative responses were observed in splenocytes from mice of most groups vaccinated with IC31(®)-adjuvanted gD, only i.d. immunization resulted in a significant splenic IFN-γ response. Further, immunization with gD plus IC31(®) conferred 80-100% protection against an otherwise lethal vaginal HSV-2 challenge with amelioration of viral replication and disease severity in the vagina. These results warrant further exploration of IC31(®) for induction of protective immunity against genital herpes and other sexually transmitted infections.

摘要

单纯疱疹病毒 2 型(HSV-2)引起的生殖器疱疹仍然是全球生殖器溃疡的主要原因。鉴于最近人类生殖器疱疹疫苗试验的结果令人失望,迫切需要开发能够诱导针对 HSV-2 的保护性粘膜和全身免疫反应的新型疫苗策略。在这里,我们测试了佐剂 IC31(®)与 HSV-2 糖蛋白 D(gD)联合使用通过鼻腔(i.n.)、皮内(i.d.)或皮下(s.c.)免疫途径在 C57BL/6 小鼠中诱导针对生殖器疱疹感染的保护性免疫的能力。通过所有三种免疫途径用 gD 和 IC31(®)免疫,可产生针对 gD 的升高的血清抗体反应,并具有中和 HSV-2 的活性。虽然皮肤途径促进了 IgG2c/IgG1 同型混合的诱导,但 i.n.途径仅诱导 IgG1 抗体。所有免疫途径均能诱导阴道中 gD 特异性 IgG 抗体反应在接种了 IC31(®)-佐剂 gD 的小鼠中。尽管用 IC31(®)-佐剂 gD 接种的大多数组的小鼠脾细胞中观察到特异性淋巴细胞增殖反应,但只有 i.d.免疫导致脾 IFN-γ 反应显著。此外,用 gD 和 IC31(®)免疫可提供 80-100%的保护,防止阴道 HSV-2 攻击的致命性,减轻阴道中的病毒复制和疾病严重程度。这些结果证明了进一步探索 IC31(®)诱导针对生殖器疱疹和其他性传播感染的保护性免疫的必要性。

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