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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:DNA初免疫苗接种后上皮增强可增强痘苗病毒的抗原表达从而产生有效的CD8 + T细胞介导的抗肿瘤免疫力

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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 (), 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重组牛痘病毒载体疫苗均在表达HPV16 / E7的肿瘤模型中引起了HPV特异性CD8 + T细胞应答,并已被用作初免加强疗法增强人乳头瘤病毒特异性免疫反应的治疗方案(),TA-HPV的最佳给药途径仍不清楚。在临床前模型中,我们检查了肌内pNGVL4a-Sig / E7(detox)/ HSP70引发的TA-HPV加强免疫后的免疫原性。我们观察到,用pNGVL4a-Sig / E7(detox)/ HSP70引发两次,然后通过皮肤划痕进行一次TA-HPV免疫增强,在C57BL / 6小鼠中产生最强的抗原特异性CD8 + T细胞应答。这些数据转化为肿瘤控制和治疗小鼠的延长生存期。我们的结果为肌内pNGVL4a-Sig / E7(排毒)/ HSP70 DNA疫苗原液,TA-HPV疫苗皮肤稀疏促进免疫方案控制HPV相关疾病的未来临床测试提供了依据。

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