Co-delivery of curcumin and resveratrol by folic acid-conjugated poly (glycerol adipate) nanoparticles for enhanced synergistic anticancer effect against osteosarcoma

被引:8
作者
Wongrakpanich, Amaraporn [1 ]
Thu, Huong Bui Thi [2 ]
Sakchaisri, Krisada [3 ]
Taresco, Vincenzo [4 ]
Crucitti, Valentina Cuzzucoli [5 ]
Bunsupa, Somnuk [6 ]
Suksiriworapong, Jiraphong [1 ]
机构
[1] Mahidol Univ, Fac Pharm, Dept Pharm, Bangkok 10400, Thailand
[2] Univ Angers, Fac Hlth, Dept Pharm, F-49100 Angers, France
[3] Mahidol Univ, Fac Pharm, Dept Pharmacol, Bangkok 10400, Thailand
[4] Univ Nottingham, Sch Chem, Nottingham NG7 2RD, England
[5] Univ Nottingham, Dept Chem & Environm Engn, Nottingham NG7 2RD, England
[6] Mahidol Univ, Fac Pharm, Dept Pharmacognosy, Bangkok 10400, Thailand
关键词
Curcumin; Resveratrol; Nanoparticle; Osteosarcoma; Co-delivery; Synergistic; IN-VITRO; DRUG-DELIVERY; COMBINATION; CANCER; ENCAPSULATION; CELLS; VIVO; CARCINOMA; MICELLES; DESIGN;
D O I
10.1016/j.jddst.2024.105610
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
This study explored the co-delivery of curcumin (CUR) and resveratrol (RV) using folic acid-conjugated poly (glycerol adipate)-based nanoparticles (FPPC NPs) to enhance their synergistic anticancer effects against osteosarcoma. Based on synergistic toxicity experiments against Saos-2 cells, the optimal synergistic CUR:RV ratios were 1:2 and 1:3, which were used for co-encapsulation. Increasing the amount of RV in the co-loaded NPs did not affect the properties of the nanocarriers, but predominantly increased the loading capacity of RV, especially at the 1:3 ratio, by 1.8-2.0 times, mediated by their interaction. All co-loaded NPs demonstrated sustained release of CUR with a burst release of RV, and the presence of RV accelerated the initial release of CUR from the carriers. Furthermore, the co-encapsulated NPs maintained CUR and RV synergism and greatly enhanced their toxicity against osteosarcoma by at least 1.8 times compared to their corresponding solutions through profound accumulation of Saos-2 cells in the sub G1 phase and late apoptosis. The internalization of FPPC NPs into cells via endocytosis was dose- and time-dependent. This study offers a proof-of-concept for a potential co-delivery system using tumor-targeted poly(glycerol adipate)-based NPs to enhance the anticancer activity of CUR and RV against osteosarcoma.
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页数:14
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