Carrier‐Free Disulfiram Based Nanomedicine for Enhanced Cancer Therapy

Author:

Dang Meng1,Lu Nan2,Shi Xuzhi3,Li Qiang4,Lin Bin5,Dong Heng4,Han Xiaolin3,Rui Jiaxin3,Sun Junfen1,Luo Wei1,Teng Zhaogang3ORCID,Su Xiaodan3

Affiliation:

1. State Key Laboratory for Modification of Chemical Fibers and Polymer Materials College of Materials Science and Engineering Institute of Functional Materials Donghua University Shanghai 201620 P.R. China

2. Department of Nuclear Medicine Zhongnan Hospital of Wuhan University Wuhan University Wuhan Hubei 430062 P. R. China

3. Key Laboratory for Organic Electronics and Information Displays and Jiangsu Key Laboratory for Biosensors Institute of Advanced Materials Jiangsu National Synergetic Innovation Centre for Advanced Materials Nanjing University of Posts and Telecommunications Nanjing Jiangsu 210023 P.R. China

4. Nanjing Stomatological Hospital Medical School Nanjing University Nanjing Jiangsu 210008 P. R. China

5. Department of Radiology Second Affiliated Hospital School of Medicine Zhejiang University Hangzhou Zhejiang 310000 P. R. China

Abstract

AbstractNumerous nanomedicines have been developed to improve the efficiency and safety of conventional anticancer drugs. However, the carrier materials and intricate nature of multifunctional design always hindered the clinical transformation of nanomedicines. Herein, a novel carrier‐free anticancer nanomedicine (CFDC) with tailored morphologies including nanodots, nanorod and nanosheet were prepared using the clinically approved anti‐alcoholism drug disulfiram (DSF) via supramolecular assembly process. Our study reveals that CFDC induces the production of reactive oxygen species and activates the downstream apoptosis‐related c‐Jun N‐terminal kinase (JNK) and p‐38 pathway. In addition, the CFDC effectively counteract the inhibitory effect of NF‐κB expression on ROS‐induced cellular cytotoxicity, ultimately resulting in enhanced cell apoptosis, which is not achievable by pure DSF and the simply mixing of DSF and Cu2+ (DSF+Cu). Notably, the CFDC exhibits 3.1‐, 3.0‐folds increased on cancer cell DNA damage compared with the DSF, and DSF+Cu groups. In vivo experiments conducted on breast‐ or prostate‐bearing mice modals demonstrated that the CFDC exhibits a higher efficacy in suppressing the tumor growth. The remarkable drug delivery efficiency and better anticancer effect of CFDC nanodrug provide promising prospects for the clinical transformation of DSF based nanodrug in cancer therapy.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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