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Significantly increased anti‐tumor activity of carcinoembryonic antigen‐specific chimeric antigen receptor T cells in combination with recombinant human IL‐12

Xiaowei ChiDevelopment Center for Medicine Science and Technology National Health and Family Planning Commission of the People's Republic of China Beijing P. R. ChinaPeiwei YangState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaErhao ZhangState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaJieyi GuState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaHui XuState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaMengwei LiState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaXinmei GaoState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaXin LiState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaYinan ZhangState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaHanmei XuState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaHanmei XuState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. ChinaJialiang HuState Key Laboratory of Natural Medicines, Ministry of Education China Pharmaceutical University Nanjing P. R. China
2019en
ABI

Аннотация

BACKGROUND AIMS: Chimeric antigen receptor T cells (CAR-T cells) have been successfully used in treatments of hematological tumors, however, their anti-tumor activity in solid tumor treatments was limited. As IL-12 increases T-cell immune functions, we designed carcinoembryonic antigen (CEA) specific CAR-T (CEA-CAR-T) cells and, for the first time, used them in combination with recombinant human IL-12 (rhIL-12) to treat several types of solid tumors. METHODS: In vitro anti-tumor activity of CEA-CAR-T cells in combination with rhIL-12 was confirmed by evaluation of CEA-CAR-T cell activation, proliferation, and cytotoxicity after co-incubation with CEA-positive or CEA-negative human tumor cells. In vivo anti-tumor activity of CEA-CAR-T cells in combination with rhIL-12 was confirmed in a xenograft model in nude mice for treatments of several types of solid tumors. RESULTS: In vitro experiments confirmed that rhIL-12 significantly increased the activation, proliferation, and cytotoxicity of CEA-CAR-T cells. Similarly, in vivo experiments found that CEA-CAR-T cells in combination with rhIL-12 had significantly enhanced anti-tumor activity than CEA-CAR-T cells in growth inhibition of newly colonized colorectal cancer cell HT-29, pancreatic cancer cell AsPC-1, and gastric cancer cell MGC803. CONCLUSIONS: These works confirmed that simultaneous use of cytokines, for example, rhIL-12, can increase the anti-tumor activity of CAR-T cells, especially for treatments of several types of solid tumors.

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