Simplified Gambogic Acid Prodrug Nanoparticles to Improve Efficiency and Reduce Toxicity for Clinical Translation Potential

Author:

Wang Ruyi1,Xiao Yuxiao1,Zhang Zhongtao2,Huang Xiaoxian2,Zhu Wanfang1,Ma Xiao3,Feng Feng24,Liu Wenyuan15,Han Lingfei1,Qu Wei2ORCID

Affiliation:

1. Department of Pharmaceutical Analysis China Pharmaceutical University Nanjing 210009 China

2. Department of Natural Medicinal Chemistry China Pharmaceutical University Nanjing 210009 China

3. State Drug Administration‐Key laboratory of Quality control of Chinese Medicinal Materials and Decoction Pieces Gansu Institute for Drug Control Lanzhou 730070 China

4. Nanjing Medical University Nanjing 211198 China

5. Zhejiang Center for Safety Study of Drug Substances Industrial Technology Innovation Platform Hangzhou 310018 China

Abstract

AbstractPoor in vivo characteristics of gambogic acid (GA) and difficulties in industrial manufacturing of its nanocarriers have hindered its clinical translation. Therefore, a reproducible nano‐drug delivery system must be developed to realize simpler manufacture and address inherent defects of GA, such as short circulation and severe side effects, in order to facilitate its clinical application. Herein, a drug self‐assembled nanoparticles (NPs) consisting of a hydrophobic prodrug based on GA and oleyl alcohol (OA), as well as vitamin E‐polyethylene glycol succinate (TPGS) as a shield to improve the stability of the NPs is reported. The preparation method is simple enough to stably facilitate large‐scale manufacturing. The self‐assembled NPs exhibit a remarkably high drug‐loading capacity, and their prolonged circulation enables the NPs to demonstrate superior antitumor efficacy in both cellular and animal models. The flexible hydrophobic long chain wraps GA groups, which mitigates vascular irritation and reduces hemolysis rates. Consequently, the prodrug nano‐system addresses GA‐related concerns regarding stability, efficacy, and safety, offering a simple, stable, and secure nano‐platform for similar candidate drugs.

Funder

China Postdoctoral Science Foundation

Natural Science Foundation of Jiangsu Province

National Natural Science Foundation of China

Publisher

Wiley

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