New Approach in Ocular Drug Delivery: In vitro and ex vivo Investigation of Cyclodextrin-Containing, Mucoadhesive Eye Drop Formulations

Bíró, Tivadar; Bocsik, Alexandra; Dukovski, Bisera Jurišić; Gróf, Ilona; Lovrić, Jasmina; Csóka, Ildikó; Deli, Mária A.; Aigner, Zoltán

doi:10.2147/dddt.s264745

Cited by 6 publications

(4 citation statements)

References 36 publications

(52 reference statements)

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“…After 30 min of treatment, cell viability was measured. The results showed no sign of cytotoxicity [ 48 ]. ZnHA (0.15%) is also used in a commercially available eye drop.…”

Section: Discussionmentioning

confidence: 99%

Design and Optimization of In Situ Gelling Mucoadhesive Eye Drops Containing Dexamethasone

Szalai

Jójárt-Laczkovich

Kovács

et al. 2022

Gels

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Poor bioavailability of eye drops is a well-known issue, which can be improved by increasing the residence time on the eye surface and the penetration of the active pharmaceutical ingredient (API). This study aims to formulate in situ gelling mucoadhesive ophthalmic preparations. To increase the residence time, the formulations were based on a thermosensitive polymer (Poloxamer 407 (P407)) and were combined with two types of mucoadhesive polymers. Dexamethasone (DXM) was solubilized by complexation with cyclodextrins (CD). The effect of the composition on the gel structure, mucoadhesion, dissolution, and permeability was investigated with 33 full factorial design. These parameters of the gels were measured by rheological studies, tensile test, dialysis membrane diffusion, and in vitro permeability assay. The dissolution and permeability of the gels were also compared with DXM suspension and CD-DXM solution. The gelation is strongly determined by P407; however, the mucoadhesive polymers also influenced it. Mucoadhesion increased with the polymer concentration. The first phase of drug release was similar to that of the CD-DXM solution, then it became prolonged. The permeability of DXM was significantly improved. The factorial design helped to identify the most important factors, thereby facilitating the formulation of a suitable carrier for the CD-DXM complex.

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“…After 30 min of treatment, cell viability was measured. The results showed no sign of cytotoxicity [ 48 ]. ZnHA (0.15%) is also used in a commercially available eye drop.…”

Section: Discussionmentioning

confidence: 99%

Design and Optimization of In Situ Gelling Mucoadhesive Eye Drops Containing Dexamethasone

Szalai

Jójárt-Laczkovich

Kovács

et al. 2022

Gels

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“…Statens Seruminstitut rabbit corneal cells (SIRC) and HCE-T (human corneal epithelial cell-transformed cell line) cells are the most commonly used immortalized cells in corneal toxicology, transport, and permeability research. ,,− The SIRC cell line was the first immortalized cell line derived from corneal tissue. Although, these cells have been isolated from rabbit corneas in 1957, their origin is unknown, and there are no records of their first 400 passages .…”

Section: In Vitro Reconstructed Corneal Tissue Models To Study Drug P...mentioning

confidence: 99%

“…The limitation of this model is that it does not include the stroma or endothelial cells. As pointed out by Bíro et al, who compared the uptake of cyclodextrins in an in vitro epithelial corneal model and an ex vivo diffusion cell, permeability was substantially higher in the in vitro model, because this model only contained the corneal epithelium . Furthermore, another drawback is that the wing cells and basal cells in the cultured epithelium are not as well organized as they are in the intact cornea, this is significant since appropriate organization of these cells is necessary for maintaining the cornea’s integrity and function…”

Section: In Vitro Reconstructed Corneal Tissue Models To Study Drug P...mentioning

confidence: 99%

In Vitro and Ex Vivo Models for Assessing Drug Permeation across the Cornea

et al. 2023

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Drug permeation across the cornea remains a major challenge due to its unique and complex anatomy and physiology. Static barriers such as the different layers of the cornea, as well as dynamic aspects such as the constant renewal of the tear film and the presence of the mucin layer together with efflux pumps, all present unique challenges for effective ophthalmic drug delivery. To overcome some of the current ophthalmic drug limitations, the identification and testing of novel drug formulations such as liposomes, nanoemulsions, and nanoparticles began to be considered and widely explored. In the early stages of corneal drug development reliable in vitro and ex vivo alternatives, are required, to be in line with the principles of the 3Rs (Replacement, Reduction, and Refinement), with such methods being in addition faster and more ethical alternatives to in vivo studies. The ocular field remains limited to a handful of predictive models for ophthalmic drug permeation. In vitro cell culture models are increasingly used when it comes to transcorneal permeation studies. Ex vivo models using excised animal tissue such as porcine eyes are the model of choice to study corneal permeation and promising advancements have been reported over the years. Interspecies characteristics must be considered in detail when using such models. This review updates the current knowledge about in vitro and ex vivo corneal permeability models and evaluates their advantages and limitations.

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“…Ex vivo corneal permeability across freshly excised rabbit cornea was investigated using the membrane diffusion method [43]. Briefly, the excised cornea was sandwiched between the donor and receptor compartments of Franz diffusion cell.…”

Section: Ex Vivo Corneal Permeability Studymentioning

confidence: 99%

Development of Carvedilol Nanoformulation-Loaded Poloxamer-Based In Situ Gel for the Management of Glaucoma

Almutairy,

Khafagy,

Abu Lila

2023

Gels

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The objective of the current study was to fabricate a thermosensitive in situ gelling system for the ocular delivery of carvedilol-loaded spanlastics (CRV-SPLs). In situ gel formulations were prepared using poloxamer analogs by a cold method and was further laden with carvedilol-loaded spanlastics to boost the precorneal retention of the drug. The gelation capacity, rheological characteristics, muco-adhesion force and in vitro release of various in situ gel formulations (CS-ISGs) were studied. The optimized formula (F2) obtained at 22% w/v poloxamer 407 and 5% w/v poloxamer 188 was found to have good gelation capacity at body temperature with acceptable muco-adhesion properties, appropriate viscosity at 25 °C that would ease its ocular application, and relatively higher viscosity at 37 °C that promoted prolonged ocular residence of the formulation post eye instillation and displayed a sustained in vitro drug release pattern. Ex vivo transcorneal penetration studies through excised rabbit cornea revealed that F2 elicited a remarkable (p ˂ 0.05) improvement in CRV apparent permeation coefficient (Papp = 6.39 × 10−6 cm/s) compared to plain carvedilol-loaded in situ gel (CRV-ISG; Papp = 2.67 × 10−6 cm/s). Most importantly, in normal rabbits, the optimized formula (F2) resulted in a sustained intraocular pressure reduction and a significant enhancement in the ocular bioavailability of carvedilol, as manifested by a 2-fold increase in the AUC0–6h of CRV in the aqueous humor, compared to plain CRV-ISG formulation. To sum up, the developed thermosensitive in situ gelling system might represent a plausible carrier for ophthalmic drug delivery for better management of glaucoma.

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New Approach in Ocular Drug Delivery: In vitro and ex vivo Investigation of Cyclodextrin-Containing, Mucoadhesive Eye Drop Formulations

Cited by 6 publications

References 36 publications

Design and Optimization of In Situ Gelling Mucoadhesive Eye Drops Containing Dexamethasone

Design and Optimization of In Situ Gelling Mucoadhesive Eye Drops Containing Dexamethasone

In Vitro and Ex Vivo Models for Assessing Drug Permeation across the Cornea

Development of Carvedilol Nanoformulation-Loaded Poloxamer-Based In Situ Gel for the Management of Glaucoma

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