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Induction of multispecific Th-1 type immune response against HCV in mice by protein immunization using CpG and Montanide ISA 720 as adjuvants

机译:使用CpG和Montanide ISA 720作为佐剂的蛋白免疫诱导小鼠针对HCV的多特异性Th-1型免疫应答

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摘要

Recent studies demonstrate that Th1-type immune responses against a broad spectrum of hepatitis C virus (HCV) gene products are crucial to the resolution of acute HCV infection. We investigated new vaccine approaches to augment the strength of HCV-specific Th1-type immune responses. ELISPOT assay revealed that single or multiple protein immunization using both CpG ODN and Montanide ISA 720 as adjuvants induced much stronger IFN-γ-producing Th1 responses against core, NS3 and NS5b targets than did the formulation without these adjuvants. Protein vaccination using CpG ODN and Montanide ISA 720 as adjuvants also greatly enhanced humoral responses to HCV core, E1/E2 and NS3. When specific IgG isotypes were assayed, protein immunization using CpG ODN and Montanide ISA 720 as adjuvants produced higher titers of IgG2a dominant antibodies than did protein immunization alone, indicating a more Th1-biasedpathway. This increase in IgG2a is consistent with the induction of Th1 cells secreting IFN-γ demonstrated by ELISPOT assay. In conclusion, protein immunization using CpG ODN and Montanide ISA 720 as adjuvants greatly enhanced cellular (Th1 type) as well as humoral immune responses against HCV in Balb/c mice. The use of adjuvants appears critical to the induction of Th1 immune responses during HCV vaccination with recombinant proteins.
机译:最近的研究表明,针对广泛的丙型肝炎病毒(HCV)基因产物的Th1型免疫应答对于解决急性HCV感染至关重要。我们研究了新的疫苗方法,以增强HCV特异性Th1型免疫应答的强度。 ELISPOT分析表明,与不含这些佐剂的制剂相比,使用CpG ODN和Montanide ISA 720作为佐剂的单种或多种蛋白质免疫诱导的针对核心,NS3和NS5b靶标的IFN-γ产生性Th1反应强得多。使用CpG ODN和Montanide ISA 720作为佐剂的蛋白质疫苗接种也大大增强了对HCV核心,E1 / E2和NS3的体液反应。当分析特定的IgG同种型时,使用CpG ODN和Montanide ISA 720作为佐剂的蛋白免疫产生的IgG2a优势抗体效价要高于单独的蛋白免疫,表明Th1偏向的途径更多。 IgG2a的这种增加与ELISPOT分析显示诱导Th1细胞分泌IFN-γ一致。总之,使用CpG ODN和Montanide ISA 720作为佐剂的蛋白质免疫极大地增强了Balb / c小鼠的针对HCV的细胞(Th1型)以及体液免疫反应。佐剂的使用对于用重组蛋白进行HCV疫苗接种期间诱导Th1免疫应答显得至关重要。

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