首页> 外文期刊>Vaccine >Recombinant heat shock protein 65 carrying PADRE and HBV epitopes activates dendritic cells and elicits HBV-specific CTL responses.
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Recombinant heat shock protein 65 carrying PADRE and HBV epitopes activates dendritic cells and elicits HBV-specific CTL responses.

机译:携带PADRE和HBV表位的重组热休克蛋白65激活树突状细胞并引发HBV特异性CTL反应。

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摘要

BCG Hsp65 and PADRE have been shown to be potent to enhance antigen specific immunity. In order to explore the possibility to utilize them for the development of HBV therapeutic vaccine, a chimeric protein, Hsp65-HBV, was created by fusing PADRE and epitopes from HBV to the carboxyl-terminus of BCG Hsp65 and expressed in E. coli. We evaluated its effects on human dendritic cell maturation and specific CTL induction in vitro. Results showed that Hsp65-HBV could activate human dendritic cells by up-regulating the expressions of HLA-A2, HLA-DR and CD86, companioning with high level of IL-12 secretion. Furthermore, Hsp65-HBV matured DCs could significantly stimulate human autologous CD8+ T cell proliferation and induce HBV-specific CTLs. Hsp65-HBV was also shown to generate HBsAg-specific CTLs in vivo in mice. These results indicated that Hsp65-HBV might be a candidate for the treatment of chronic HBV infection.Digital Object Identifier http://dx.doi.org/10.1016/j.vaccine.2010.12.124
机译:已显示BCG Hsp65和PADRE可有效增强抗原特异性免疫。为了探索将它们用于开发HBV治疗疫苗的可能性,通过将PADRE和表位从HBV融合到BCG Hsp65的羧基末端来创建嵌合蛋白Hsp65-HBV,并在E中表达。大肠杆菌。我们评估了其对人树突状细胞成熟和体外特定CTL诱导的影响。结果表明,Hsp65-HBV可以通过上调HLA-A2,HLA-DR和CD86的表达来激活人树突状细胞,并伴随高水平的IL-12分泌。此外,Hsp65-HBV成熟的DC可以显着刺激人自体CD8 + T细胞的增殖并诱导HBV特异性CTL。还显示出Hsp65-HBV在小鼠体内可体内产生HBsAg特异性CTL。这些结果表明,Hsp65-HBV可能是治疗慢性HBV感染的候选药物。数字对象标识符http://dx.doi.org/10.1016/j.vaccine.2010.12.124

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