Targeting Alpha-Fetoprotein (AFP)–MHC Complex with CAR T-Cell Therapy for Liver Cancer

抗原 嵌合抗原受体 癌症研究 免疫疗法 医学 人类白细胞抗原 癌症 肿瘤抗原 癌症免疫疗法 主要组织相容性复合体 生物 免疫学 内科学 免疫系统 T细胞
作者
Hong Liu,Yiyang Xu,Jingyi Xiang,Li Long,Shon Green,Zhiyuan Yang,Bryan Zimdahl,Jingwei Lu,Neal Cheng,Lucas H. Horan,Bin Liu,Su Yan,Pei Wang,Juan E. Diaz,Lu Jin,Yoko Nakano,Javier F. Morales,Pengbo Zhang,Lian-xing Liu,Binnaz K. Staley,Saul J. Priceman,Christine E. Brown,Stephen J. Forman,Vivien W. Chan,Liu C
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:23 (2): 478-488 被引量:185
标识
DOI:10.1158/1078-0432.ccr-16-1203
摘要

Abstract Purpose: The majority of tumor-specific antigens are intracellular and/or secreted and therefore inaccessible by conventional chimeric antigen receptor (CAR) T-cell therapy. Given that all intracellular/secreted proteins are processed into peptides and presented by class I MHC on the surface of tumor cells, we used alpha-fetoprotein (AFP), a specific liver cancer marker, as an example to determine whether peptide–MHC complexes can be targets for CAR T-cell therapy against solid tumors. Experimental Design: We generated a fully human chimeric antigen receptor, ET1402L1-CAR (AFP-CAR), with exquisite selectivity and specificity for the AFP158–166 peptide complexed with human leukocyte antigen (HLA)-A*02:01. Results: We report that T cells expressing AFP-CAR selectively degranulated, released cytokines, and lysed liver cancer cells that were HLA-A*02:01+/AFP+ while sparing cells from multiple tissue types that were negative for either expressed proteins. In vivo, intratumoral injection of AFP-CAR T cells significantly regressed both Hep G2 and AFP158-expressing SK-HEP-1 tumors in SCID-Beige mice (n = 8 for each). Moreover, intravenous administration of AFP-CAR T cells in Hep G2 tumor-bearing NSG mice lead to rapid and profound tumor growth inhibition (n = 6). Finally, in an established intraperitoneal liver cancer xenograft model, AFP-CAR T cells showed robust antitumor activity (n = 6). Conclusions: This study demonstrates that CAR T-cell immunotherapy targeting intracellular/secreted solid tumor antigens can elicit a potent antitumor response. Our approach expands the spectrum of antigens available for redirected T-cell therapy against solid malignancies and offers a promising new avenue for liver cancer immunotherapy. Clin Cancer Res; 23(2); 478–88. ©2016 AACR.

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