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首页> 外文期刊>Biological research: BR >Recombinant in vitro assembled hepatitis C virus core particles induce strong specific immunity enhanced by formulation with an oil-based adjuvant
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Recombinant in vitro assembled hepatitis C virus core particles induce strong specific immunity enhanced by formulation with an oil-based adjuvant

机译:重组体外组装的丙型肝炎病毒核心颗粒可诱导强大的特异性免疫,通过与油基佐剂一起配制可增强免疫力

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摘要

In the present work, immunogenicity of recombinant in vitro assembled hepatitis C virus core particles, HCcAg.120-VLPs, either alone or in combination with different adjuvants was evaluated in BALB/c mice. HCcAg.120-VLPs induced high titers of anti-HCcAg.120 antibodies and virus-specific cellular immune responses. Particularly, HCcAg.120-VLPs induced specific delayed type hypersensitivity, and generated a predominant T helper 1 cytokine pro file in immunized mice. In addition, HCcAg.120-VLPs prime splenocytes proliferate in vitro against different HCcAg.120-specific peptides, depending on either the immunization route or the adjuvant used. Remarkably, immunization with HCcAg.120-VLPs/Montanide ISA888 formulation resulted in a significant control of vaccinia virus titer in mice after challenge with a recombinant vaccinia virus expressing HCV core protein, vvCore. Animals immunized with this formulation had a marked increase in the number of IFN-γ producing spleen cells, after stimulation with P815 cells infected with vvCore. These results suggest the use of recombinant HCV core particles as components of therapeutic or preventive vaccine candidates against HCV.
机译:在本工作中,在BALB / c小鼠中评估了重组体外组装的丙型肝炎病毒核心颗粒HCcAg.120-VLP的免疫原性,无论是单独使用还是与不同佐剂组合使用。 HCcAg.120-VLP诱导出高滴度的抗HCcAg.120抗体和病毒特异性细胞免疫应答。特别是,HCcAg.120-VLPs诱导了特异性的迟发型超敏反应,并在免疫小鼠中产生了主要的T辅助1细胞因子。另外,HCcAg.120-VLPs脾细胞在体外针对不同的HCcAg.120特异性肽增殖,这取决于所使用的免疫途径或佐剂。值得注意的是,用表达HCV核心蛋白vvCore的重组痘苗病毒攻击后,用HCcAg.120-VLP / Montanide ISA888制剂免疫可显着控制小鼠痘苗病毒的滴度。用vvCore感染的P815细胞刺激后,用这种制剂免疫的动物脾脏中产生IFN-γ的细胞数量明显增加。这些结果表明使用重组HCV核心颗粒作为针对HCV的治疗或预防性疫苗候选物的成分。

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