Pharmacokinetics of the aldose reductase inhibitor imirestat following topical ocular administration

Pharmacokinetics of the aldose reductase inhibitor imirestat following topical ocular administration

The pharmacokinetics of imirestat following topical ocular administration were evaluated in a series of studies in rabbits and dogs. Following single topical doses to both albino and pigmented rabbits, imirestat was subject to rapid uptake into the cornea followed by an initial rapid decline and the...

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Bibliographic Details
Published in:Pharmaceutical research Vol. 7; no. 2; pp. 192 - 198
Main Authors: BRAZZELL, R. K, WOOLDRIDGE, C. B, HACKETT, R. B, MCCUE, B. A
Format: Journal Article
Language:English
Published: New York, NY Springer 01-02-1990
Subjects:
Administration, Topical
Aldehyde Reductase - antagonists & inhibitors
Animals
Biological and medical sciences
Biological Availability
Dogs
Eye
Fluorenes - administration & dosage
Fluorenes - pharmacokinetics
Hydantoins - administration & dosage
Hydantoins - pharmacokinetics
Hydrogen-Ion Concentration
Medical sciences
Pharmacology. Drug treatments
Rabbits
Sugar Alcohol Dehydrogenases - antagonists & inhibitors
Tissue Distribution
Multiple dose
Eye
Aldose reductase
Animal
Single dose
Enzyme inhibitor
Bioavailability
Pharmacokinetics
Intraocular administration
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Summary:The pharmacokinetics of imirestat following topical ocular administration were evaluated in a series of studies in rabbits and dogs. Following single topical doses to both albino and pigmented rabbits, imirestat was subject to rapid uptake into the cornea followed by an initial rapid decline and then very slow elimination, with a t1/2 of approximately 130 hr. Drug was rapidly absorbed into aqueous humor, with concentrations declining to nondetectable levels by 12 hr. Imirestat was retained in the lens following topical dosing similar to that in cornea, with an apparent elimination t1/2 of 140 hr. Vitreous humor concentrations of drug were detectable for up to 72 hr after dosing. There was no apparent difference in the disposition of the drug between albino and pigmented rabbits. Bioavailability following topical dosing increased with dose, although not in a linear fashion. Formulation pH did not have an appreciable effect on ocular bioavailability. There was detectable systemic absorption following topical dosing, with plasma concentrations in rabbit being 50 to 75% of that observed following an equivalent intravenous dose. However, drug levels in the dosed eyes were significantly higher than in contralateral undosed eyes. Multiple dosing of imirestat for 6 weeks resulted in accumulation of drug in rabbit lens. Concentrations were higher in lens cortex than lens nucleus, with the time course for accumulation being different for the two. Our data suggest that imirestat penetrates into ocular tissue following topical dosing and is retained in lens and cornea, potential sites of action for the drug.
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content type line 23
ISSN:0724-8741
1573-904X
DOI:10.1023/A:1015893122054