Erlotinib and curcumin-loaded nanoparticles embedded in thermosensitive chitosan hydrogels for enhanced treatment of head and neck cancer

被引:0
|
作者
Haider, Mohamed [1 ,2 ]
Jagal, Jayalakshmi [2 ]
Alghamdi, Maha Ali [3 ,4 ]
Haider, Youssef [5 ]
Hassan, Hatem A. F. M. [6 ,7 ]
Najm, Muna B. [2 ]
Jayakuma, Manju N. [2 ]
Ezzat, Helal [8 ,9 ]
Greish, Khaled [4 ]
机构
[1] Univ Sharjah, Coll Pharm, Dept Pharmaceut & Pharmaceut Technol, Sharjah 27272, U Arab Emirates
[2] Univ Sharjah, Res Inst Med & Hlth Sci, Sharjah 27272, U Arab Emirates
[3] Taif Univ, Coll Sci, Dept Biotechnol, Taif 21974, Saudi Arabia
[4] Arabian Gulf Univ, Princess Al Jawhara Ctr Mol Med, Sch Med & Med Sci, Dept Mol Med, Manama 329, Bahrain
[5] Boston Univ, Coll Engn, Boston, MA USA
[6] Univ Kent, Medway Sch Pharm, Cent Ave, Canterbury ME4 4TB, England
[7] Cairo Univ, Fac Pharm, Dept Pharmaceut & Ind Pharm, Cairo 11562, Egypt
[8] Univ Sharjah, Res Inst Sci & Engn, Sharjah 27272, U Arab Emirates
[9] Delta Higher Inst Engn & Technol, Civil Engn Dept, Mansoura, Egypt
关键词
Tyrosine kinase inhibitors; Head and neck cancer; Controlled release; PLGA nanoparticles; Thermosensitive hydrogels; Curcumin; CONTROLLED DRUG-DELIVERY; IN-VITRO EVALUATION; CELL LUNG-CANCER; PLGA NANOPARTICLES; BIODEGRADABLE NANOPARTICLES; FORMULATION; RELEASE; SYSTEM; GEFITINIB; THERAPY;
D O I
10.1016/j.ijpharm.2024.124825
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Head and neck squamous cell carcinoma (HNSCC) remain a major oncological challenge with significant morbidity and mortality rates. Erlotinib (Er) and Curcumin (Cm) are potential therapeutic agents for HNSCC, yet they are hindered by poor solubility and bioavailability. This study explored the optimization of poly(lactic-coglycolic acid) nanoparticles co-loaded with Er and Cm (Er/Cm-NP), prepared via a D-optimal response surface design-guided nanoprecipitation process. The optimized formulation, optEr/Cm-NP, was then incorporated into chitosan/beta-glycerophosphate hydrogels (optEr/Cm-NP-HG) to create an injectable intratumoral (IT) nanocomposite hydrogel (HG) delivery system. Physicochemical properties of the formulations, including gelation time, injectability, mechanical strength and drug release profiles were assessed alongside hemolytic activity. Compared to optEr/Cm-NP alone, the NP-loaded HG formulation exhibited a more pronounced modulation effect, enabling sustained and controlled drug release. The cytotoxicity of the developed formulations was evaluated using the FaDu HNSCC cancer cell line. Both optEr/Cm-NP and optEr/Cm-NP-HG21 displayed enhanced cytotoxicity compared to free drugs. Confocal laser microscopy and flow cytometry confirmed superior cellular uptake of Er and Cm when delivered via NPs or NP-loaded HG. Furthermore, a significant increase in apoptotic cell death upon treatment with optEr/Cm-NP was observed, highlighting its potential for HNSCC therapy. In vivo studies conducted on a xenograft HNSCC mouse model revealed the significant capacity of the intratumorallyinjected optEr/Cm-NP-HG21 formulation to retard the tumor growth. Conclusively, the results presented herein report the successful development of a nanocomposite HG system incorporating NPs co-loaded with Er and Cm that could be efficiently utilized in the treatment of HNSCC.
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收藏
页数:22
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