丙型肝炎病毒多表位抗原在小鼠与家兔中的免疫应答

在丙型肝炎病毒 (hepatitisCvirus,HCV)基因组中优选 5个具有良好免疫原性的高度保守T/B细胞表位 ,组合成一个HCV多表位抗原基因 ,并与β 半乳糖苷酶基因融合后在E .coli中高效表达了具有HCV免疫特异性的GZ PCX抗原 .纯化的蛋白质免疫小鼠与家兔后 ,诱发了高滴度 ( 10 -6)的抗 GZ PCXIgG ,并可在高水平上维持数月 .弗氏完全佐剂与死减毒鼠伤寒沙门氏菌均可发挥高效的佐剂效应 .用GZ PCX抗原及其表位多肽刺激后 ,可诱发较高水平的特异性CTL应答、迟发性超敏反应及淋巴细胞增殖 .在免疫小鼠的肠道灌洗液中可检测到抗 GZ PCXsIgG .免疫后小鼠未见明显的毒副反应 ,具有良好的安全性 ,可望发展一种针对不同型。

Specific immune responses induced by a multi-epitope antigen of hepatitis C virus in mice and rabbits

Five highly conserved and immunogenic epitopes of hepatitis C virus (HCV) have been chosen to form a multi-epitope antigen gene and fused with β-galactosidase gene to express a hybrid GZ-PCX antigen, which could be specifically recognized by human HCV sera. High level of anti-GZ-PCX IgG has been induced when mice or rabbits were immunized with GZ-PCX antigen emulsificated with complete Freund’s adjuvant or mixed with killed attenuated Salmonella typhimurium SL3261. The specific anti-GZ-PCX IgG reached a high liter of 10-6, which remained for several months. Specific cytotoxic T lymphocyte (CTL) effects, delayed type hypersensltivity reaction (DTH) and proliferation of peripheral lymphocytes have been induced by GZ-PCX antigen or synthetic peptides. High level of anti-GZ-PCX slgG has been detected in mice’s intestinal washing fluids, which indicates that the antigen induced mucosal immunity as well as systematic immunity. The studies show that the HCV multi-epitope antigen induces high level of specific immune responses without obvious toxicity, which might be able to provide protectivity to any HCV genotypes and isolates.