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American Journal of PharmTech Research

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Optimization of the In Vitro Transcorneal Release and the In Vivo IOP-Lowering Effects of Latanoprost Ophthalmic Gel Formulations Using Azone™ as a Penetration Enhancer and Carbopol-974® as a Mucoadhesive

Published in February 2014 Issue 1 (Vol. 4, Issue 1, 2014)

Optimization of the In Vitro Transcorneal Release and the In Vivo IOP-Lowering Effects of Latanoprost Ophthalmic Gel Formulations Using Azone™ as a Penetration Enhancer and Carbopol-974® as a Mucoadhesive - Issue cover

Abstract

The objectives of this study were to maximize; a) the in vitro transcorneal release, b) the IOP-lowering effect and, c) the duration of action, of Latanoprost acid (LAT) ophthalmic gels. The in vitro transcorneal release of LAT from a 1st set of gel formulations that containing different concentrations of Azone™ (as enhancer) with fixed concentration of C-974® (as mucoadhesive) were studied. Formulation that showed greatest permeability parameters at lowest Azone™ concentration was selected for preparation of a 2nd set of ocular gels containing various C-974® concentrations. The in vitro transcorneal release was assessed, and the best C-974® concentration required for preparation of formulations that can be conceded as ideal ophthalmic LAT gels hve been pinpointed and scaled up for in vivo IOP-lowering efficacy study using TONO-PEN™ AVIA tonometer in rabbits for 4-consecutive days.  Various test formulations have showed significant but varied augmentations in both, in vitro and in vivo results. Formulations (GAZ-4) & GC-4 have shown the highest therapeutic IOP lowering effects; i.e., (7.8±1.8), (6.5±2.1), respectively. Particularly noteworthy with both formulations the IOP base-line didn’t re-established after 24 hours, and their durations of action in the single-dose study were 47±2.25, and 48±1.5, respectively. The in vitro release, onset, magnitude & duration of action of action of LAT gels have been enhanced and extended for up to 2-day with two gel formulations.  Nonetheless, the success in developing a novel ophthalmic formulation depended for great extent upon the crucial net outcomes of a very sensitive interplay/balance between the drug and additives.

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Article Information

Article ID:
AJPTR41052
Paper ID:
AJPTR-01-001932
Published Date:
2014-02-01

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How to Cite

Afouna & Naim (2014). Optimization of the In Vitro Transcorneal Release and the In Vivo IOP-Lowering Effects of Latanoprost Ophthalmic Gel Formulations Using Azone™ as a Penetration Enhancer and Carbopol-974® as a Mucoadhesive. American Journal of PharmTech Research, 4(1), xx-xx. https://ajptr.scholarjms.com/articles/994

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