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首页> 外文期刊>The journal of immunology >IL-12 Delivery from Recombinant Vaccinia Virus Attenuates the Vector and Enhances the Cellular Immune Response Against HIV-1 Env in a Dose-Dependent Manner
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IL-12 Delivery from Recombinant Vaccinia Virus Attenuates the Vector and Enhances the Cellular Immune Response Against HIV-1 Env in a Dose-Dependent Manner

机译:从重组痘苗病毒的IL-12传递减弱了载体,并以剂量​​依赖的方式增强了针对HIV-1 Env的细胞免疫反应。

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To develop vaccination strategies against HIV-1 infection aimed to specifically enhance the cell-mediated immunity (CMI), we have engineered vaccinia virus (VV) recombinants expressing HIV-1 Env (rVVenv) and murine IL-12 (rVVlucIL-12) genes or coexpressing both genes (rVVenvIL-12). In mice inoculated with rVVlucIL-12 there is a rapid clearance of the virus, and this correlates with the induction of high levels of IL-12 and IFN-γ in serum and spleen early after infection. Enzyme-linked immunospot analysis of mice inoculated with rVVlucIL-12, revealed a nearly 2-fold increase in the number of specific anti-VV CD8+ T cells compared with that in mice given control rVV, and the serum Ab response was biased in favor of a Th1 response. An enhancement of about 2-fold in the number of anti-gp160 IFN-γ-secreting CD8+ T cells was observed in mice inoculated with rVVenvIL-12, when a dose of 1 × 107 PFU/mouse was used, but this enhancement was not observed when mice were given 5 × 107 PFU. This variation with virus dosage was confirmed in mice immunized simultaneously with different multiplicities of rVV expressing singly the env or IL-12 genes. The highest specific CMI was obtained in mice coadministered a low dose (2 × 104 PFU) of rVVlucIL-12 and 1 × 107 PFU of rVVenv. Our findings provide evidence for specific enhancement of the CMI to HIV-1 Env by the differential expression of IL-12 and env genes delivered from VV recombinants. This approach can be of wide vaccination interest as a means to improve immune responses to other Ags.
机译:为了开发针对HIV-1感染的疫苗接种策略,以专门增强细胞介导的免疫(CMI),我们设计了表达HIV-1 Env(rVVenv)和鼠IL-12(rVVlucIL-12)基因的牛痘病毒(VV)重组体或共表达两个基因(rVVenvIL-12)。在用rVVlucIL-12接种的小鼠中,病毒迅速清除,这与感染后早期在血清和脾脏中诱导高水平的IL-12和IFN-γ有关。接种rVVlucIL-12的小鼠的酶联免疫斑点分析显示,与给予对照rVV的小鼠相比,特异性抗VV CD8 + T细胞的数量增加了近2倍,并且血清Ab反应偏向于Th1反应。使用1×107 PFU /小鼠的剂量接种rVVenvIL-12的小鼠中观察到分泌抗gp160IFN-γ的CD8 + T细胞数量增加了约2倍,但没有这种增加当给小鼠5×107 PFU时观察到。在用分别表达env或IL-12基因的不同多重性rVV同时免疫的小鼠中证实了病毒剂量的这种变化。在低剂量(2×104 PFU)的rVVlucIL-12和1×107 PFU的rVVenv共同给药的小鼠中获得了最高的特异性CMI。我们的发现为通过VV重组子传递的IL-12和env基因的差异表达,将CMI特异性增强到HIV-1 Env提供了证据。这种方法可能会引起广泛的疫苗接种兴趣,作为改善对其他Ags免疫反应的一种手段。

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