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首页> 外文期刊>Virology >Epithelial boost enhances antigen expression by vaccinia virus for the generation of potent CD8+T cell-mediated antitumor immunity following DNA priming vaccination
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Epithelial boost enhances antigen expression by vaccinia virus for the generation of potent CD8+T cell-mediated antitumor immunity following DNA priming vaccination

机译:上皮提升通过疫苗病毒增强抗原表达,用于产生效率的CD8 + T细胞介导的抗肿瘤免疫接种疫苗

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摘要

While both pNGVL4a-Sig/E7(detox)/HSP70 DNA vaccine and TA-HPV recombinant vaccinia viral vector-based vaccines have elicited HPV-specific CD8 + T cell responses in HPV16/E7-expressing tumor models, and been used as prime-boost regimen to enhance HPV-specific immune responses in humans (NCT00788164), the optimal route of administration for TA-HPV remains unclear. In a preclinical model, we examined the immunogenicity of priming with intramuscular pNGVL4a-Sig/E7(detox)/HSP70 followed by TA-HPV boost through different administration routes. We observed that priming twice with a pNGVL4a-Sig/E7(detox)/HSP70 followed by a single TA-HPV immunization boost through skin scarification generated the strongest antigen specific CD8 + T cell response in C57BL/6 mice. These data translate to tumor control and prolonged survival of treated mice. Our results provide rationale for future clinical testing of intramuscular pNGVL4a-Sig/E7(detox)/HSP70 DNA vaccine prime, TA-HPV vaccine skin scarification boost immunization regimen for the control of HPV-associated diseases.
机译:虽然Pngvl4a-sig / E7(Detox)/ Hsp70 DNA疫苗和TA-HPV重组疫苗病毒载体的疫苗引发了HPV16 / E7表达肿瘤模型中的HPV特异性CD8 + T细胞反应,并被用作素数 - 增强人类的HPV特异性免疫应答的增强方案(NCT00788164),TA-HPV的最佳给药途径尚不清楚。在临床前模型中,我们检查了用肌内Pngv14A-Sig / E7(Detox)/ Hsp70引发的免疫原性,然后通过不同的给药路线进行TA-HPV。我们观察到,用Pngvl4a-sig / E7(Detox)/ Hsp70的灌注两次,然后通过皮肤吞吐产生的单一TA-HPV免疫促进,在C57BL / 6小鼠中产生最强的抗原特异性CD8 + T细胞反应。这些数据转化为肿瘤对照和治疗小鼠的延长存活。我们的结果为未来的肌内PNGVL4A-SIG / E7(DETOX)/ HSP70 DNA疫苗粉末素,TA-HPV疫苗皮肤造成促进免疫制度来控制HPV相关疾病的临床检测。

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