An Injectable Puerarin Depot Can Potentiate Chimeric Antigen Receptor Natural Killer Cell Immunotherapy Against Targeted Solid Tumors by Reversing Tumor Immunosuppression

Author:

Liu Yan1ORCID,Hao Yu2,Chen Jiahui1,Chen Minming2,Tian Jia1,Lv Xiang1,Zhang Yefei1,Ma Xinxing3,Zhou Yehui4,Feng Liangzhu2ORCID

Affiliation:

1. Jiangsu Key Laboratory for Molecular and Medical Biotechnology Cancer Institute Department of Biochemistry College of Life Science Nanjing Normal University Nanjing 210023 P. R. China

2. Institute of Functional Nano & Soft Materials (FUNSOM) Jiangsu Key Laboratory for Carbon‐Based Functional Materials & Devices Soochow University 199 Ren'ai Road Suzhou 215123 P. R. China

3. Department of Radiology The First Affiliated Hospital of Soochow University Suzhou 215006 P. R. China

4. Department of General Surgery The First Affiliated Hospital of Soochow University Suzhou 215000 P. R. China

Abstract

AbstractChimeric antigen receptor natural killer (CAR‐NK) cell therapy represents a potent approach to suppressing tumor growth because it has simultaneously inherited the specificity of CAR and the intrinsic generality of NK cells in recognizing cancer cells. However, its therapeutic potency against solid tumors is still restricted by insufficient tumor infiltration, immunosuppressive tumor microenvironments, and many other biological barriers. Motivated by the high potency of puerarin, a traditional Chinese medicine extract, in dilating tumor blood vessels, an injectable puerarin depot based on a hydrogen peroxide‐responsive hydrogel comprising poly(ethylene glycol) dimethacrylate and ferrous chloride is concisely developed. Upon intratumoral fixation, the as‐prepared puerarin depot (abbreviated as puerarin@PEGel) can activate nitrogen oxide production inside endothelial cells and thus dilate tumor blood vessels to relieve tumor hypoxia and reverse tumor immunosuppression. Such treatment can thus promote tumor infiltration, survival, and effector functions of customized epidermal growth factor receptor (HER1)‐targeted HER1‐CAR‐NK cells after intravenous administration. Consequently, such puerarin@PEGel‐assisted HER1‐CAR‐NK cell treatment exhibits superior tumor suppression efficacy toward both HER1‐overexpressing MDA‐MB‐468 and NCI‐H23 human tumor xenografts in mice without inducing obvious side effects. This study highlights a potent strategy to activate CAR‐NK cells for augmented treatment of targeted solid tumors through reprogramming tumor immunosuppression.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Jiangsu Province

Collaborative Innovation Center of Suzhou Nano Science and Technology

Publisher

Wiley

Subject

Biomaterials,Biotechnology,General Materials Science,General Chemistry

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