Accurate control of dual-receptor-engineered T cell activity through a bifunctional anti-angiogenic peptide

Erhao Zhang; Jieyi Gu; Jianpeng Xue; Chenyu Lin; Chen Liu; Mengwei Li; Jingchao Hao; Sarra Setrerrahmane; Xiaowei Chi; Weiyan Qi; Jialiang Hu; Hanmei Xu

doi:10.1186/s13045-018-0591-7

Accurate control of dual-receptor-engineered T cell activity through a bifunctional anti-angiogenic peptide

J Hematol Oncol. 2018 Mar 20;11(1):44. doi: 10.1186/s13045-018-0591-7.

Authors

Erhao Zhang¹, Jieyi Gu¹, Jianpeng Xue^{1

2}, Chenyu Lin¹, Chen Liu¹, Mengwei Li¹, Jingchao Hao^{1

3}, Sarra Setrerrahmane¹, Xiaowei Chi¹, Weiyan Qi^{1

2}, Jialiang Hu^{4

5}, Hanmei Xu^{6

7

8}

Affiliations

¹ The Engineering Research Center of Peptide Drug Discovery and Development, China Pharmaceutical University, Nanjing, 210009, People's Republic of China.
² State Key Laboratory of Natural Medicines, Ministry of Education, China Pharmaceutical University, Nanjing, 210009, People's Republic of China.
³ School of Pharmaceutical Sciences and Yunnan Provincial Key Laboratory of Pharmacology for Natural Products, Kunming Medical University, Kunming, 650500, People's Republic of China.
⁴ The Engineering Research Center of Peptide Drug Discovery and Development, China Pharmaceutical University, Nanjing, 210009, People's Republic of China. jialiang_hu51@aliyun.com.
⁵ State Key Laboratory of Natural Medicines, Ministry of Education, China Pharmaceutical University, Nanjing, 210009, People's Republic of China. jialiang_hu51@aliyun.com.
⁶ The Engineering Research Center of Peptide Drug Discovery and Development, China Pharmaceutical University, Nanjing, 210009, People's Republic of China. 13913925346@126.com.
⁷ State Key Laboratory of Natural Medicines, Ministry of Education, China Pharmaceutical University, Nanjing, 210009, People's Republic of China. 13913925346@126.com.
⁸ Nanjing Anji Biotechnology Co., Ltd., Nanjing, 210046, People's Republic of China. 13913925346@126.com.

Abstract

Background: Chimeric antigen receptors (CARs) presented on T cell surfaces enable redirection of T cell specificity, which has enormous promise in antitumor therapy. However, excessive activity and poor control over such engineered T cells cause significant safety challenges, such as cytokine release syndrome and organ toxicities. To enhance the specificity and controllable activity of CAR-T cells, we report a novel switchable dual-receptor CAR-engineered T (sdCAR-T) cell and a new switch molecule of FITC-HM-3 bifunctional molecule (FHBM) in this study.

Methods: We designed a fusion molecule comprising FITC and HM-3. HM-3, an antitumor peptide including an Arg-Gly-Asp sequence, can specifically target integrin αvβ3 that is presented on some tumor cells. Moreover, to improve the specificity of CAR-T cells, we also generated the sdCAR-T cell line against cognate tumor cells expressing human mesothelin (MSLN) and integrin αvβ3. Finally, the activity of sdCAR-T cell and FHBM is verified via in vitro and in vivo experiments.

Results: In the presence of FHBM, the designed sdCAR-T cells exerted high activity including activation and proliferation and had specific cytotoxicity in a time- and dose-dependent manner in vitro. Furthermore, using a combination of FHBM in nude mice, sdCAR-T cells significantly inhibited the growth of MSLN⁺ K562 cells and released lower levels of the cytokines (e.g., interleukin-2, interferon γ, interleukin-6, and tumor necrosis factor α) relative to conventional CAR-T cells, obtaining specific, controllable, and enhanced cytotoxicity.

Conclusions: Our data indicate that FHBM can accurately control timing and dose of injected CAR-T cells, and sdCAR-T cells exert significant antitumor activity while releasing lower levels of cytokines for the cognate tumor cells expressing both MSLN and integrin αvβ3. Therefore, combination therapies using sdCAR-T cells and the switch molecule FHBM have significant potential to treat malignancies.

Keywords: Bifunctional molecule; Cancer immunotherapy; HM-3; K562 cell; Switchable dual-receptor CAR.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Angiogenic Proteins / immunology*
Animals
Humans
Mesothelin
Mice
Receptors, Chimeric Antigen / immunology*
T-Lymphocytes / immunology*

Substances

Angiogenic Proteins
MSLN protein, human
Msln protein, mouse
Receptors, Chimeric Antigen
Mesothelin