工程化靶向 E7 的 T 细胞在小鼠模型中介导人乳头瘤病毒癌症消退。
Engineered T cells targeting E7 mediate regression of human papillomavirus cancers in a murine model.
机构信息
Experimental Transplantation and Immunology Branch, National Cancer Institute, NIH, Bethesda, Maryland, USA.
Kite Pharma, Amsterdam, Netherlands.
出版信息
JCI Insight. 2018 Apr 19;3(8). doi: 10.1172/jci.insight.99488.
Abstract
T cell receptor (TCR) T cell therapy is a promising cancer treatment modality. However, its successful development for epithelial cancers may depend on the identification of high-avidity TCRs directed against tumor-restricted target antigens. The human papillomavirus (HPV) E7 antigen is an attractive therapeutic target that is constitutively expressed by HPV+ cancers but not by healthy tissues. It is unknown if genetically engineered TCR T cells that target E7 can mediate regression of HPV+ cancers. We identified an HPV-16 E7-specific, HLA-A*02:01-restricted TCR from a uterine cervix biopsy from a woman with cervical intraepithelial neoplasia. This TCR demonstrated high functional avidity, with CD8 coreceptor-independent tumor targeting. Human T cells transduced to express the TCR specifically recognized and killed HPV-16+ cervical and oropharyngeal cancer cell lines and mediated regression of established HPV-16+ human cervical cancer tumors in a mouse model. These findings support the therapeutic potential of this approach and established the basis for an E7 TCR gene therapy clinical trial in patients with metastatic HPV+ cancers (NCT02858310).
摘要
T 细胞受体 (TCR) T 细胞疗法是一种很有前途的癌症治疗方法。然而,要将其成功开发用于上皮癌,可能取决于能否鉴定出针对肿瘤受限靶抗原的高亲和力 TCR。人乳头瘤病毒 (HPV) E7 抗原是一个很有吸引力的治疗靶点,HPV+癌症持续表达该抗原,但健康组织不表达。目前尚不清楚针对 E7 的基因工程 TCR T 细胞是否能介导 HPV+癌症消退。我们从一名患有宫颈上皮内瘤变的女性的宫颈活检中鉴定出一种 HPV-16 E7 特异性、HLA-A*02:01 限制性 TCR。这种 TCR 表现出高功能亲和力,无需 CD8 共受体即可靶向肿瘤。转导表达 TCR 的人 T 细胞特异性识别并杀伤 HPV-16+宫颈和口咽癌细胞系,并介导已建立的 HPV-16+人宫颈癌肿瘤在小鼠模型中的消退。这些发现支持了这种方法的治疗潜力,并为转移性 HPV+癌症患者的 E7 TCR 基因治疗临床试验奠定了基础(NCT02858310)。
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