当在HIV感染中使用乙肝疫苗时，CpG可增加疫苗抗原特异性细胞介导免疫。

Journal of immune based therapies and vaccines Pub Date : 2008-08-12 DOI:10.1186/1476-8518-6-4

Jonathan B Angel, Curtis L Cooper, Jennifer Clinch, Charlene D Young, Andreane Chenier, Karl G Parato, Michael Lautru, Heather Davis, Donald W Cameron

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引用次数: 33

摘要

背景:缺乏足够的佐剂是疫苗缺乏免疫原性的一个可能的解释。免疫刺激性CpGs是有效的疫苗佐剂，可能是开发疫苗的重要组成部分，特别是那些需要细胞免疫反应来保护的疫苗。我们之前已经证明，CpG ODN与乙肝疫苗联合使用在HIV感染个体中导致对乙肝表面抗原更早、更强和更持久的抗体反应，并且希望确定在该人群中，辅助性t细胞反应是否也得到增强。方法:我们在乙型肝炎易感、有效治疗的hiv血清阳性个体中进行了一项双盲、安慰剂对照试验。参与者在第0,4和8周接受乙肝疫苗，安慰剂或CPG 7909 1.0 mg。为了确定CpG对细胞免疫反应的影响，在基线和第4、8、12、24和48周时，通过[3H]-胸腺嘧啶掺入来评估淋巴细胞增殖反应(LPR)。淋巴细胞亚群的免疫表型也在这些时间点确定。结果:入选的36例患者中，18例单独接种乙肝疫苗，18例联合CpG接种乙肝疫苗。纳入CPG 7909与初始接种后所有时间点对HBsAg的更大增殖反应相关。在8周(p = 0.042)和48周(p = 0.024)时，这种增加具有统计学意义。当LPR作为刺激指数(SI)评估时，也观察到类似的结果。对HIV p24 Ag的增殖反应没有观察到差异，淋巴细胞亚群也没有任何差异。结论:除了增强对疫苗的体液应答外，我们首次描述了CPG 7909在典型的低应答人群中增强对疫苗抗原的细胞免疫。这种佐剂在开发需要细胞免疫应答保护的有效疫苗中可能是重要的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

CpG increases vaccine antigen-specific cell-mediated immunity when administered with hepatitis B vaccine in HIV infection.

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CpG increases vaccine antigen-specific cell-mediated immunity when administered with hepatitis B vaccine in HIV infection.

Background: Lack of adequate adjuvancy is a possible explanation for lack of vaccine immunogenecity. Immunostimulatory CpGs are potent vaccine adjuvants and may be an important component of the development vaccines, particularly those for which a cellular immune response is required for protection. We have previously demonstrated that CpG ODN co-administration with hepatitis B vaccine results in earlier, stronger and more sustained antibody responses to hepatitis B surface antigen in HIV infected individuals, and wished to determine if, in this population, helper T-cell responses were also enhanced.

Methods: We conducted a double-blind, placebo-controlled trial in hepatitis B susceptible, effectively treated HIV-seropositive individuals. Participants received hepatitis B vaccine, with either placebo or CPG 7909 1.0 mg at week 0, 4 and 8. To determine the impact of CpG on cellular immune responses, lymphoproliferative responses (LPR) were evaluated by [3H]-thymidine incorporation at baseline and weeks 4, 8, 12, 24, and 48. Immunophenotyping of lymphocyte subsets was also determined at these time points.

Results: Of 36 patients enrolled, 18 received hepatitis B vaccine alone, and 18 received hepatitis B vaccine with CpG. Inclusion of CPG 7909 was associated with a greater proliferative response to HBsAg at all time points following initial vaccination. This increase was statistically significant at 8 weeks (p = 0.042) and 48 weeks (p = 0.024). Similar results were observed when LPR were evaluated as stimulation indices (SI). No differences in proliferative responses to HIV p24 Ag were observed, nor were there any differences in lymphocyte subsets.

Conclusion: In addition to enhancing humoral responses to vaccination, we describe for the first time that CPG 7909 enhances cellular immunity to vaccine antigen in a typically hyporesponsive population. This adjuvancy may be important in the development of an effective vaccine for which a cellular immune response is required for protection.

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Journal of immune based therapies and vaccines

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