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A novel CD4 T-cell epitope described from one of the cervical cancer patients vaccinated with HPV 16 or 18 E7-pulsed dendritic cells

机译:从一名接受HPV 16或18 E7脉冲树突状细胞疫苗接种的宫颈癌患者中描述的新型CD4 T细胞表位

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摘要

Previously, safety and immunogenicity of human papillomavirus type 16 (HPV16) or 18 E7-pulsed dendritic cells (DC) vaccinations were demonstrated in a dose-escalation Phase I clinical trial which enrolled ten patients diagnosed with stage IB or IIA cervical cancer (nine HPV 16-positive, one HPV 18-positive). The goal of the study was to define the T-cell epitopes of HPV 16 or 18 E7 protein in these patients in order to develop new strategies for treating HPV-associated malignancies. This was accomplished through establishing T-cell lines by stimulating peripheral blood mononuclear cells with autologous mature DC pulsed with the HPV 16 or 18 E7 protein, examining the T-cell responses using ELISPOT assays, and isolating E7-specific T-cell clones based on IFN-γ secretion. Then, the epitope was characterized in terms of its core sequence and the restriction element. Twelve T-cell lines from eight subjects (seven HPV 16-positive, one HPV 18-positive) were evaluated. Positive T-cell responses were demonstrated in four subjects (all HPV 16-positive). All four were positive for the HPV 16 E7 46–70 (EPDRAHYNIVTFCCKCDSTLRLCVQ) region. T-cell clones specific for the E7 47–70 region were isolated from one of the subjects. Further analyses revealed a novel, naturally processed, CD4 T-cell epitope, E7 58–68 (CCKCDSTLRLC), restricted by the HLA-DR17 molecule.
机译:以前,在剂量递增的I期临床试验中证实了16型人乳头瘤病毒(HPV16)或18 E7脉冲树突状细胞(DC)疫苗的安全性和免疫原性,该试验招募了十名诊断为IB或IIA期宫颈癌的患者(9例HPV 16阳性,一个HPV 18阳性)。该研究的目的是确定这些患者中HPV 16或18 E7蛋白的T细胞表位,以开发治疗HPV相关恶性肿瘤的新策略。这是通过以下方法完成的:建立T细胞系,方法是用HPV 16或18 E7蛋白脉冲的自体成熟DC刺激外周血单核细胞,使用ELISPOT分析检测T细胞反应,并分离基于E7的E7特异性T细胞克隆IFN-γ分泌。然后,根据其核心序列和限制元件表征表位。评价了来自八个受试者的十二个T细胞系(七个HPV 16阳性,一个HPV 18阳性)。在四名受试者(所有HPV 16阳性)中证实了阳性T细胞应答。这四个区域的HPV 16 E7 46-70(EPDRAHYNIVTFCCKCDSTLRLCVQ)均为阳性。从一名受试者中分离出对E7 47-70区域特异的T细胞克隆。进一步的分析揭示了一种新的,自然加工的CD4 T细胞表位,E7 58-68(CCKCDSTLRLC),受HLA-DR17分子限制。

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