Abstract
Glaucoma is one of the leading causes of irreversible blindness worldwide. It is characterized by progressive optic neuropathy in association with damage to the optic nerve head and, subsequently, visual loss if it is left untreated. Among the drug classes used for the long-term treatment of open-angle glaucoma, prostaglandin analogues (PGAs) are the first-line treatment and are available as marketed eye drop formulations for intraocular pressure (IOP) reduction by increasing the trabecular and uveoscleral outflow. PGAs have low aqueous solubility and are very unstable (i.e., hydrolysis) in aqueous solutions, which may hamper their ocular bioavailability and decrease their chemical stability. Additionally, treatment with PGA in conventional eye drops is associated with adverse effects, such as conjunctival hyperemia and trichiasis. It has been a very challenging for formulation scientists to develop stable aqueous eye drop formulations that increase the PGAs’ solubility and enhance their therapeutic efficacy while simultaneously lowering their ocular side effects. Here the physiochemical properties and chemical stabilities of the commercially available PGAs are reviewed, and the compositions of their eye drop formulations are discussed. Furthermore, the novel PGA formulations for glaucoma treatment are reviewed.
Funder
Faculty of Pharmaceutical Sciences, Chulalongkorn University
Reference81 articles.
1. Molecular Genetics of Glaucoma: Subtype and Ethnicity Considerations
2. Factors for Glaucoma Progression and the Effect of Treatment
3. Prostaglandins;Sali,2005
4. Prostaglandins: A general review;Shaw;Res. Prostaglandins,1971
5. Reduction of intraocular pressure by prostaglandins applied topically to the eyes of conscious rabbits;Camras;Investig. Ophthalmol. Vis. Sci.,1977
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