Anti-cancer effect of fenbendazole-incorporated PLGA nanoparticles in ovarian cancer

Chi-son Chang; Ji-yoon Ryu; June-kuk Choi; Young-jae Cho; Jung-joo Choi; Jae Ryoung Hwang; Ju-yeon Choi; Joseph J Noh; Chan Mi Lee; Ji Eun Won; Hee Dong Han; Jeong-won Lee

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Anti-cancer effect of fenbendazole-incorporated PLGA nanoparticles in ovarian cancer

Author: Chi-Son CHANG ¹ ; Ji-Yoon RYU ; June-Kuk CHOI ; Young-Jae CHO ; Jung-Joo CHOI ; Jae Ryoung HWANG ; Ju-Yeon CHOI ; Joseph J. NOH ; Chan Mi LEE ; Ji Eun WON ; Hee Dong HAN ; Jeong-Won LEE
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1. Department of Obstetrics and Gynecology, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul, Korea
Publication Type:Original Article
From:Journal of Gynecologic Oncology 2023;34(5):e58-
CountryRepublic of Korea
Language:English
Abstract: Objective:Fenbendazole (FZ) has potential anti-cancer effects, but its poor water solubility limits its use for cancer therapy. In this study, we investigated the anti-cancer effect of FZ with different drug delivery methods on epithelial ovarian cancer (EOC) in both in vitro and in vivo models.
Methods:EOC cell lines were treated with FZ and cell proliferation was assessed. The effect of FZ on tumor growth in cell line xenograft mouse model of EOC was examined according to the delivery route, including oral and intraperitoneal administration. To improve the systemic delivery of FZ by converting fat-soluble drugs to hydrophilic, we prepared FZ-encapsulated poly(D,L-lactide-co-glycolide) acid (PLGA) nanoparticles (FZ-PLGA-NPs). We investigated the preclinical efficacy of FZ-PLGA-NPs by analyzing cell proliferation, apoptosis, and in vivo models including cell lines and patient-derived xenograft (PDX) of EOC.
Results:FZ significantly decreased cell proliferation of both chemosensitive and chemoresistant EOC cells. However, in cell line xenograft mouse models, there was no effect of oral FZ treatment on tumor reduction. When administered intraperitoneally, FZ was not absorbed but aggregated in the intraperitoneal space. We synthesized FZ-PLGA-NPs to obtain water solubility and enhance drug absorption. FZ-PLGA-NPs significantly decreased cell proliferation in EOC cell lines. Intravenous injection of FZ-PLGA-NP in xenograft mouse models with HeyA8 and HeyA8-MDR significantly reduced tumor weight compared to the control group. FZ-PLGA-NPs showed anti-cancer effects in PDX model as well.
Conclusion:FZ-incorporated PLGA nanoparticles exerted significant anti-cancer effects in EOC cells and xenograft models including PDX. These results warrant further investigation in clinical trials.