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Coadministration of a plasmid encoding HIV-1 Gag enhances the efficacy of cancer DNA vaccines

机译:共同施用编码HIV-1 Gag的质粒增强了癌症DNa疫苗的功效

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摘要

DNA vaccination holds great promise for the prevention and treatment of cancer and infectious diseases. However, the clinical ability of DNA vaccines is still controversial due to the limited immune response initially observed in humans. We hypothesized that electroporation of a plasmid encoding the HIV-1 Gag viral capsid protein would enhance cancer DNA vaccine potency. DNA electroporation used to deliver plasmids in vivo, induced type I interferons, thereby supporting the activation of innate immunity. The coadministration of ovalbumin (OVA) and HIV-1 Gag encoding plasmids modulated the adaptive immune response. This strategy favored antigen-specific Th1 immunity, delayed B16F10-OVA tumor growth and improved mouse survival in both prophylactic and therapeutic vaccination approaches. Similarly, a prophylactic DNA immunization against the melanoma-associated antigen gp100 was enhanced by the codelivery of the HIV-1 Gag plasmid. The adjuvant effect was not driven by the formation of HIV-1 Gag virus-like particles. This work highlights the ability of both electroporation and the HIV-1 Gag plasmid to stimulate innate immunity for enhancing cancer DNA vaccine immunogenicity and demonstrates interesting tracks for the design of new translational genetic adjuvants to overcome the current limitations of DNA vaccines in humans.
机译:DNA疫苗接种对于癌症和传染病的预防和治疗具有广阔的前景。然而,由于最初在人类中观察到的有限的免疫反应,DNA疫苗的临床能力仍存在争议。我们假设,编码HIV-1 Gag病毒衣壳蛋白的质粒的电穿孔会增强癌症DNA疫苗的效力。用于体内传递质粒的DNA电穿孔诱导了I型干扰素,从而支持先天免疫的激活。卵清蛋白(OVA)和HIV-1 Gag编码质粒的共同给药调节了适应性免疫应答。这种策略有利于抗原特异性Th1免疫,延迟的B16F10-OVA肿瘤生长以及在预防性和治疗性疫苗接种方法中改善小鼠存活率。同样,HIV-1 Gag质粒的代码传递增强了针对黑色素瘤相关抗原gp100的预防性DNA免疫。辅助作用不受HIV-1 Gag病毒样颗粒形成的驱动。这项工作突出了电穿孔和HIV-1 Gag质粒刺激先天免疫以增强癌症DNA疫苗免疫原性的能力,并展示了设计新的翻译遗传佐剂以克服人类DNA疫苗目前的局限性的有趣途径。

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