pH-tailored delivery of a multitarget anticancer benzimidazole derivative using a PEGylated β-cyclodextrin-curcumin functionalized nanocomplex

被引:2
作者
Shawky, Heba [1 ]
Fayed, Dalia B. [1 ]
Ibrahim, Noha E. [2 ]
机构
[1] Natl Res Ctr, Pharmaceut Ind & Drug Res Inst, Therapeut Chem Dept, Dokki 12622, Cairo, Egypt
[2] Natl Res Ctr, Biotechnol Res Inst, Microbial Biotechnol Dept, Dokki 12622, Cairo, Egypt
来源
BIOMATERIALS ADVANCES | 2024年 / 163卷
关键词
Benzimidazole; Polymeric nanocomplex; Curcumin; beta-Cyclodextrin; Multitarget-anticancer; Drug delivery; INCLUSION COMPLEXES; DRUG-DELIVERY; SOLID-STATE; NANOPARTICLES; GROWTH; PEG; TEMPERATURE; PLGA;
D O I
10.1016/j.bioadv.2024.213964
中图分类号
TB3 [工程材料学]; R318.08 [生物材料学];
学科分类号
0805 ; 080501 ; 080502 ;
摘要
In this study, we aimed to enhance the bioavailability of a benzimidazole derivative with potent anticancer potential through a nano-based approach. Benzimidazole-loaded polyethylene glycol-beta-cyclodextrin-functionalized curcumin nanocomplex (BMPE-Cur) was prepared and characterized for its physicochemical properties and drug release profiles under different pH conditions. In addition, the biological activities of the nanocomplex including antioxidant potentials and pro-apoptogenic properties, against HepG2, PC3, and the chemo-resistant MCF-7-ADR cell lines relative to the normal Wi-38 cell line were in vitro assessed and compared with those of the free benzimidazole compound. In addition to FTIR, XRD, and NMR spectral studies, a polymeric nanocomplex with an average particle size of 467.7 nm and high stability was successfully developed, as indicated by the negative zeta potential (-28.24 mV). The nanocomplex also showed prolonged pH-sensitive sustained drug release under conditions that replicated the tumor's extra/intracellular pH. The formulated nanocomplex also demonstrated potent radical scavenging capacity owing to the inclusion of curcumin, a known radical quencher. In addition, compared with the free compound, BMPE-Cur induced DNA fragmentation-driven cell cycle arrest in HepG2, PC3, and MCF-7-ADR cells at the G1/S, G1 & S phases; respectively, with remarkable selectivity. In conclusion, the newly formulated BMPE-Cur nanocomplex represents an attractive multitarget anticancer candidate.
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页数:18
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