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IL-12 DNA 作为分子疫苗佐剂可增强 SIV DNA 疫苗接种恒河猴的细胞毒性 T 细胞反应和体液免疫反应的广度。

IL-12 DNA as molecular vaccine adjuvant increases the cytotoxic T cell responses and breadth of humoral immune responses in SIV DNA vaccinated macaques.

机构信息

Human Retrovirus Pathogenesis Section; Frederick National Laboratory for Cancer Research, Frederick, MD, USA.

出版信息

Hum Vaccin Immunother. 2012 Nov 1;8(11):1620-9. doi: 10.4161/hv.21407. Epub 2012 Aug 16.

Abstract

Intramuscular injection of macaques with an IL-12 expression plasmid (0.1 or 0.4 mg DNA/animal) optimized for high level of expression and delivered using in vivo electroporation, resulted in the detection of systemic IL-12 cytokine in the plasma. Peak levels obtained by day 4-5 post injection were paralleled by a rapid increase of IFN-γ, indicating bioactivity of the IL-12 cytokine. Both plasma IL-12 and IFN-γ levels were reduced to basal levels by day 14, indicating a short presence of elevated levels of the bioactive IL-12. The effect of IL-12 as adjuvant together with an SIVmac239 DNA vaccine was further examined comparing two groups of rhesus macaques vaccinated in the presence or absence of IL-12 DNA. The IL-12 DNA-adjuvanted group developed significantly higher SIV-specific cellular immune responses, including IFN-γ (+) Granzyme B (+) T cells, demonstrating increased levels of vaccine-induced T cells with cytotoxic potential, and this difference persisted for 6 mo after the last vaccination. Coinjection of IL-12 DNA led to increases in Gag-specific CD4 (+) and CD4 (+) CD8 (+) double-positive memory T cell subsets, whereas the Env-specific increases were mainly mediated by the CD8 (+) and CD4 (+) CD8 (+) double-positive memory T cell subsets. The IL-12 DNA-adjuvanted vaccine group developed higher binding antibody titers to Gag and mac251 Env, and showed higher and more durable neutralizing antibodies to heterologous SIVsmE660. Therefore, co-delivery of IL-12 DNA with the SIV DNA vaccine enhanced the magnitude and breadth of immune responses in immunized rhesus macaques, and supports the inclusion of IL-12 DNA as vaccine adjuvant.

摘要

给猕猴肌肉内注射经过优化以实现高水平表达的 IL-12 表达质粒(0.1 或 0.4mg DNA/动物),并用体内电穿孔法递送,导致在血浆中检测到系统性的 IL-12 细胞因子。在注射后第 4-5 天达到的峰值水平与 IFN-γ 的快速增加平行,表明 IL-12 细胞因子具有生物活性。在第 14 天,血浆中 IL-12 和 IFN-γ 水平均降至基础水平,表明生物活性的 IL-12 水平存在时间较短。进一步检查了 IL-12 作为佐剂与 SIVmac239 DNA 疫苗一起的作用,比较了两组在存在或不存在 IL-12 DNA 的情况下接种 rhesus 猕猴的 SIVmac239 DNA 疫苗。IL-12 DNA 佐剂组发展出明显更高的 SIV 特异性细胞免疫反应,包括 IFN-γ(+)Granzyme B(+)T 细胞,表明具有细胞毒性潜能的疫苗诱导 T 细胞水平增加,这种差异在最后一次接种后持续了 6 个月。IL-12 DNA 的共注射导致 Gag 特异性 CD4(+)和 CD4(+)CD8(+)双阳性记忆 T 细胞亚群的增加,而 Env 特异性增加主要由 CD8(+)和 CD4(+)CD8(+)双阳性记忆 T 细胞亚群介导。IL-12 DNA 佐剂疫苗组对 Gag 和 mac251 Env 的结合抗体滴度更高,并对异源 SIVsmE660 显示出更高和更持久的中和抗体。因此,将 IL-12 DNA 与 SIV DNA 疫苗共同递送增强了免疫猕猴的免疫反应的幅度和广度,并支持将 IL-12 DNA 作为疫苗佐剂纳入。

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