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Clearance of persistent HPV infection and cervical lesion by therapeutic DNA vaccine in CIN3 patients

机译:通过治疗性DNA疫苗清除CIN3患者的持续性HPV感染和宫颈病变

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摘要

Here, we demonstrate that electroporation-enhanced immunization with a rationally designed HPV DNA vaccine (GX-188E), preferentially targeting HPV antigens to dendritic cells, elicits a significant E6/E7-specific IFN-γ-producing T-cell response in all nine cervical intraepithelial neoplasia 3 (CIN3) patients. Importantly, eight out of nine patients exhibit an enhanced polyfunctional HPV-specific CD8 T-cell response as shown by an increase in cytolytic activity, proliferative capacity and secretion of effector molecules. Notably, seven out of nine patients display complete regression of their lesions and viral clearance within 36 weeks of follow up. GX-188E administration does not elicit serious vaccine-associated adverse events at all administered doses. These findings indicate that the magnitude of systemic polyfunctional CD8 T-cell response is the main contributing factor for histological, cytological and virological responses, providing valuable insights into the design of therapeutic vaccines for effectively treating persistent infections and cancers in humans.
机译:在这里,我们证明了采用合理设计的HPV DNA疫苗(GX-188E)优先针对树突状细胞靶向HPV抗原的电穿孔增强免疫,在所有9种细胞中均引起了明显的产生E6 / E7特异性IFN-γ的T细胞应答宫颈上皮内瘤变3(CIN3)患者。重要的是,每9名患者中就有8名表现出增强的多功能HPV特异性CD8 T细胞反应,如细胞溶解活性,增殖能力和效应分子分泌的增加所表明。值得注意的是,九分之七的患者在随访36周内显示出病变和病毒清除率完全消退。在所有给药剂量下,GX-188E给药均不会引起严重的疫苗相关不良事件。这些发现表明,系统性多功能CD8 T细胞应答的程度是组织学,细胞学和病毒学应答的主要因素,为有效设计治疗人类持续感染和癌症的治疗性疫苗提供了宝贵的见识。

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