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针对 HPV16/18 基因型的二价治疗性疫苗，由人纤连蛋白外域 A 与 HPV16/18 E7 病毒抗原之间的融合蛋白组成。

Bivalent therapeutic vaccine against HPV16/18 genotypes consisting of a fusion protein between the extra domain A from human fibronectin and HPV16/18 E7 viral antigens.

机构信息

Formune, Pamplona, Navarra, Spain.

Programa de Inmunología e Inmunoterapia, Centro de Investigación Médica Aplicada, University of Navarra, IdisNA, Pamplona, Navarra, Spain.

出版信息

J Immunother Cancer. 2020 Jun;8(1). doi: 10.1136/jitc-2020-000704.

DOI:10.1136/jitc-2020-000704

PMID:32581060

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7319778/

Abstract

BACKGROUND

In vivo targeting of human papillomavirus (HPV) derived antigens to dendritic cells might constitute an efficient immunotherapeutic strategy against cervical cancer. In previous works, we have shown that the extra domain A from murine fibronectin (mEDA) can be used to target antigens to toll-like receptor 4 (TLR4) expressing dendritic cells and induce strong antigen-specific immune responses. In the present study, we have produced a bivalent therapeutic vaccine candidate consisting of the human EDA (hEDA) fused to E7 proteins from HPV16 and HPV18 (hEDA-HPVE7-16/18) and evaluate its potential as a therapeutic vaccine against cervical cancer.

MATERIALS AND METHODS

Recombinant fusion proteins containing HPV E7 proteins from HPV16 and HPV18 virus subtypes fused to hEDA were produced and tested in vitro on their capacity to bind TLR4 and induce the production of tumor necrosis factor-α or interleukin (IL)-12 by human monocytes and dendritic cells. The immunogenicity and potential therapeutic activity of the vaccine in combination with cisplatin or with the TLR3 agonist molecules polyinosinic-polycytidylic acid (Poly IC) or Poly ICLC was evaluated in mice bearing subcutaneous or genital orthotopic HPV16 TC-1 tumors.

RESULTS

hEDA-HPVE7-16/18 prototype vaccine binds human TLR4 and stimulate TLR4-dependent signaling pathways and IL-12 production by human monocyte-derived dendritic cell. Vaccination with hEDA-HPVE7-16/18 induced strong HPVE7-specific Cytotoxic T lymphocyte (CTL) responses and eliminated established tumors in the TC-1-based tumor model. The antitumor efficacy was significantly improved by combining the fusion protein with cisplatin or with the TLR-3 ligand Poly IC and especially with the stabilized analog Poly ICLC. Moreover, hEDA-HPVE7-16/18+Poly ICLC induced full tumor regression in 100% of mice bearing orthotopic genital HPV tumors.

CONCLUSION

Our results suggest that this therapeutic vaccine formulation may be an effective treatment for cervical tumors that do not respond to current therapies.

摘要

背景

将人乳头瘤病毒（HPV）衍生抗原靶向递送至树突状细胞可能构成针对宫颈癌的有效免疫治疗策略。在之前的工作中，我们已经表明，来自鼠纤维连接蛋白的额外结构域 A（mEDA）可用于将抗原靶向表达 Toll 样受体 4（TLR4）的树突状细胞，并诱导强烈的抗原特异性免疫反应。在本研究中，我们生产了一种由人 EDA（hEDA）与 HPV16 和 HPV18 的 E7 蛋白融合而成的双价治疗性疫苗候选物（hEDA-HPVE7-16/18），并评估了其作为宫颈癌治疗性疫苗的潜力。

材料和方法

生产了包含 HPV16 和 HPV18 病毒亚型 E7 蛋白与 hEDA 融合的重组融合蛋白，并在体外测试其与 TLR4 结合的能力，以及诱导人单核细胞和树突状细胞产生肿瘤坏死因子-α或白细胞介素（IL）-12 的能力。在皮下或生殖部位 HPV16 TC-1 肿瘤的荷瘤小鼠中，评估了该疫苗与顺铂联合或与 TLR3 激动剂聚肌苷酸-聚胞苷酸（Poly IC）或 Poly ICLC 联合的免疫原性和潜在治疗活性。

结果

hEDA-HPVE7-16/18 原型疫苗与人 TLR4 结合并刺激 TLR4 依赖性信号通路和人单核细胞衍生树突状细胞产生 IL-12。接种 hEDA-HPVE7-16/18 可诱导强烈的 HPV E7 特异性细胞毒性 T 淋巴细胞（CTL）反应，并消除 TC-1 肿瘤模型中已建立的肿瘤。该融合蛋白与顺铂或 TLR-3 配体 Poly IC 联合，特别是与稳定化类似物 Poly ICLC 联合，显著提高了抗肿瘤疗效。此外，hEDA-HPVE7-16/18+Poly ICLC 可诱导 100%患有原位生殖 HPV 肿瘤的小鼠完全消退肿瘤。

结论

我们的结果表明，这种治疗性疫苗制剂可能是一种有效的治疗方法，可用于治疗对当前疗法无反应的宫颈肿瘤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f8db/7319778/3afd4476c4f8/jitc-2020-000704f01.jpg

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针对 HPV16/18 基因型的二价治疗性疫苗，由人纤连蛋白外域 A 与 HPV16/18 E7 病毒抗原之间的融合蛋白组成。

Bivalent therapeutic vaccine against HPV16/18 genotypes consisting of a fusion protein between the extra domain A from human fibronectin and HPV16/18 E7 viral antigens.

机构信息

出版信息

BACKGROUND

MATERIALS AND METHODS

RESULTS

CONCLUSION

背景

材料和方法

结果

结论

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