Topical noninvasive retinal drug delivery of a tyrosine kinase inhibitor: 3% cediranib maleate cyclodextrin nanoparticle eye drops in the rabbit eye

Topical noninvasive retinal drug delivery of a tyrosine kinase inhibitor: 3% cediranib maleate cyclodextrin nanoparticle eye drops in the rabbit eye

Purpose Tyrosine kinase inhibitors inhibit VEGF receptors. If delivered to the retina, they might inhibit oedema and neovascularization such as in age‐related macular degeneration and diabetic retinopathy. The aim of this study was to formulate cediranib maleate, a potent VEGF inhibitor, as γ‐cyclod...

Full description

Saved in:
Bibliographic Details
Published in:Acta ophthalmologica (Oxford, England) Vol. 100; no. 7; pp. 788 - 796
Main Authors: Lorenzo‐Soler, Laura, Praphanwittaya, Pitsiree, Olafsdottir, Olof Birna, Kristinsdottir, Iris Myrdal, Asgrimsdottir, Gudrun Marta, Loftsson, Thorsteinn, Stefansson, Einar
Format: Journal Article
Language:English
Published: England Wiley Subscription Services, Inc 01-11-2022
Subjects:
cediranib
Cyclodextrin
cyclodextrins
Diabetes mellitus
Diabetic retinopathy
Drug delivery
Drug dosages
Edema
Enzyme inhibitors
Eye
in vivo
Macular degeneration
Nanoparticles
neovascularization
Pharmacokinetics
Rabbits
Retina
Retinopathy
topical administration
Tyrosine kinase inhibitors
Vascular endothelial growth factor
Vascularization
topical administration
neovascularization
pharmacokinetics
drug delivery
cediranib
cyclodextrins
in vivo
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:Purpose Tyrosine kinase inhibitors inhibit VEGF receptors. If delivered to the retina, they might inhibit oedema and neovascularization such as in age‐related macular degeneration and diabetic retinopathy. The aim of this study was to formulate cediranib maleate, a potent VEGF inhibitor, as γ‐cyclodextrin nanoparticle eye drops and measure the retinal delivery and overall ocular pharmacokinetics after a single‐dose administration in rabbits. Methods A novel formulation technology with 3% cediranib maleate as γ‐cyclodextrin micro‐suspension was prepared by autoclaving method. Suitable stabilizers were tested for heat‐stable eye drops. The ophthalmic formulation was topically applied to one eye in rabbits. The pharmacokinetics in ocular tissues, tear film and blood samples were studied at 1, 3 and 6 hr after administration. Results γ‐cyclodextrin formed complex with cediranib maleate. The formation of γ‐cyclodextrin nanoparticles occurred in concentrated complexing media. Combined stabilizers prevented the degradation of drug during the autoclaving process. Three hours after administration of the eye drops, treated eyes showed cediranib levels of 737 ± 460 nM (mean ± SD) in the retina and 10 ± 6 nM in the vitreous humour. Conclusions Cediranib maleate in γ‐cyclodextrin nanoparticles were stable to heat in presence of stabilizers. The drug as eye drops reached the retina in concentrations that are more than 100 times higher than the 0.4 nM IC50 value reported for the VEGF type‐II receptor and thus, presumably, above therapeutic level. These results suggest that γ‐cyclodextrin‐based cediranib maleate eye drops deliver effective drug concentrations to the retina in rabbits after a single‐dose administration.
Bibliography:Laura Lorenzo‐Soler, Pitsiree Praphanwittaya (none), Olof B. Olafsdottir, Gudrun M. Asgrimsdottir and Iris M. Kristinsdottir, (employees), Thorsteinn Loftsson and Einar Stefansson (financial).
This work was supported by Oculis ehf, Reykjavík, Iceland.
ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
content type line 23
ISSN:1755-375X
1755-3768
DOI:10.1111/aos.15101