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Development and optimization of vildagliptin solid lipid nanoparticles loaded ocuserts for controlled ocular delivery: A promising approach towards treating diabetic retinopathy
Faculty
Pharmacy
Year:
2024
Type of Publication:
ZU Hosted
Pages:
Authors:
shereen Ahmed Sabry Mohamed Hosney Ismayel
Staff Zu Site
Abstract In Staff Site
Journal:
International Journal of Pharmaceutics: X ELSEVIER
Volume:
Keywords :
Development , optimization , vildagliptin solid lipid nanoparticles
Abstract:
Diabetes mellitus (DM) is the most prevalent cause of diabetic retinopathy (DRP). DRP has been recognized for a long time as a microvascular disease. Many drugs were used to treat DRP, including vildagliptin (VLD). In addition to its hypoglycemic effect, VLD minimizes ocular inflammation and improves retinal blood flow for individuals with type 2 diabetes mellitus. Nevertheless, VLD can cause upper respiratory tract infections, diarrhea, nausea, hypoglycemia, and poor tolerability when taken orally regularly due to its high water solubility and permeability. Effective ocular administration of VLD is achieved using solid lipid nanoparticles (SLNPs), which improve corneal absorption, prolonged retention, and extended drug release. Ocuserts (OCUs) are sterile, long-acting ocular dosage forms that diminish the need for frequent dosing while improving residence time and stability. Therefore, this study intends to develop VLD solid lipid nanoparticle OCUs (VLD-SLNPs-OCUs) to circumvent the issues commonly associated with VLD. SLNPs were prepared using the double-emulsion/melt dispersion technique. The optimal formula has been implemented in OCUs. Optimization and development of VLD-SLNPs-OCUs were performed using a Box-Behnken Design (BBD). VLD-SLNPs-OCUs loading efficiency was 95.28 ± 2.87%, and differential scanning calorimetry data (DSC) showed the full transformation of VLD to an amorphous state and the excellent distribution in the prepared OCUs matrices. The in vivo release of VLD from the optimized OCUs after 24 h was 35.12 ± 2.47%, consistent with in vitro drug release data of 36.89 ± 3.11. The optimized OCUs are safe to use in the eye, as shown by the ocular irritation test. VLD-SLNPs-OCUs provide extended VLD release, an advantageous alternative to conventional oral dose forms, resulting in fewer systemic adverse effects and less variation in plasma drug levels. VLD-SLNPs-OCUs might benefit retinal microvascular
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shereen Ahmed Sabry Mohamed Hosney Ismayel, "Formulation, In-Vitro and In-Vivo characterization of Vardenafil Loaded Floating In-Situ Gel: An investigational study For Enhancement of Oral Bioavailability.", Hemangi J Patel, 2017
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shereen Ahmed Sabry Mohamed Hosney Ismayel, "Gastroretentive Nizatidine Loading Microballoons for Treatment of Peptic Ulcer.", International Journal of Pharmacy and Pharmaceutical Sciences, 2015
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shereen Ahmed Sabry Mohamed Hosney Ismayel, "Formulation and in Vitro Characterization of Poly(DL-Lactide-Co-Glycolide)/Eudragit® RLPO or RS30D Nanoparticles as an Oral Carrier of Levofloxacin Hemihydrate.", TAYLOR & FRANCIS LTD, 2016
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shereen Ahmed Sabry Mohamed Hosney Ismayel, "Metoclopramide Hydrochloride Loaded Oral Wafers for Postoperative Care of Children: In vitro and In vivo Evaluation.", Bayad: AJPTR, 2019
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shereen Ahmed Sabry Mohamed Hosney Ismayel, "Enhancing Transdermal Delivery of Glimepiride Via Entrapment in Proniosomal Gel.", emanuscript services, 2016
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