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Dive into the research topics where Zora Marlowe is active.

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Featured researches published by Zora Marlowe.


Clinical Ophthalmology | 2013

Dose uniformity of loteprednol etabonate ophthalmic gel (0.5%) compared with branded and generic prednisolone acetate ophthalmic suspension (1%).

Zora Marlowe; Stephen R. Davio

Introduction Loteprednol etabonate (LE) ophthalmic gel 0.5% (Lotemax®) is a new polycarbophil-based, nonsettling topical ophthalmic formulation. The formulation is a semisolid gel at rest and a shear thinning fluid when expressed through a dropper tip. The present study was undertaken to determine how the nonsettling character of LE ophthalmic gel affects dose uniformity. Prednisolone acetate ophthalmic suspension 1% (Pred Forte®) and a generic prednisolone acetate suspension 1% were used as comparators. Methods Drug concentrations of LE ophthalmic gel, Pred Forte, and a generic prednisolone acetate suspension were determined following simulated dosing – consisting of 2 drops, expressed four times daily for 2 weeks, with bottles that were shaken or not shaken immediately prior to expressing the drops. Drug concentrations were determined using a reverse-phase high-performance liquid chromatography (HPLC) method and reported as a percentage of the declared (labeled) concentration. Comparative kinetics of drug particle sedimentation were also determined for each formulation, using dispersion analysis under gravity. Results Mean drug concentrations in drops of all three formulations were within a few percentage points of the declared concentration when the bottles were shaken for 5 seconds prior to dispensing. Only LE ophthalmic gel showed consistent and on-target concentrations when the bottles were unshaken prior to dispensing, with a mean (standard deviation [SD]) percent declared concentration of 102% (1.92%) over the 2-week dosing regimen. Drug concentrations for the branded and generic prednisolone acetate suspensions following expression from unshaken bottles were highly variable (overall relative SDs of 16.8% and 20.3%, respectively), with mean concentrations for both falling significantly below the declared concentration for drops expressed at the beginning of the 2-week dosing regimen and significantly above the declared concentration for drops expressed near the end of the dosing regimen. Dispersion analysis at 120× g showed no drug particle sedimentation for LE ophthalmic gel over the 24-hour testing period, whereas the prednisolone acetate suspensions settled in less than 6 hours. Conclusion LE ophthalmic gel 0.5% provided consistent dose uniformity at the declared concentration whether or not the bottle was shaken prior to dispensing, whereas Pred Forte® and the generic prednisolone acetate required shaking to provide consistent drug concentrations. LE ophthalmic gel may be beneficial to patients because it eliminates the potential impact on the clinical response of both under- and overdosing.


Archive | 2009

Contact Lens Solution With a Tertiary Amine Oxide

Zora Marlowe; Hongna Wang; Susan E. Burke


Archive | 2013

Ophthalmic pharmaceutical compositions and methods of making and using same

Stephen R. Davio; Paramita Sarkar; Zora Marlowe; Brian Glass; Tammy J. Kleiber


Archive | 2009

Formulations with a Tertiary Amine Oxide

Zora Marlowe; Paramita Bandyopadhyay; Hongna Wang; Eric Phillips


Archive | 2012

Pharmaceutical compositions comprising plant-based polysaccharides and uses thereof

Zora Marlowe; Paramita Sarkar; Brian Glass


Archive | 2009

Topical formulations with a tertiary amine oxide

Zora Marlowe; Paramita Bandyopadhyay; Hongna Wang; Eric Phillips


Archive | 2013

Cell protective and "wettability" enhancing properties of Hyaluronic acid + PEG 8000 in an artificial tear product

Stephen R. Davio; Megan E. Cavet; Karen Harrington; Amy Walsh; Zora Marlowe; Brian Glass; Paramita Sarkar


Archive | 2013

Compositions pharmaceutiques ophtalmiques et leurs procédés de fabrication et d'utilisation

Stephen R. Davio; Paramita Sarkar; Zora Marlowe; Brian Glass; Tammy J. Kleiber


Investigative Ophthalmology & Visual Science | 2013

A Comparative Evaluation of Lipid-based Formulations for Dry-Eye Therapy using a Corneal Epithelial Cell Desiccation Model and Physicochemical Measurements

Paramita Sarkar; Zora Marlowe; Amy Walsh; Brian Glass; Tammy J. Kleiber; Megan E. Cavet; Karen Harrington; Stephen R. Davio


Investigative Ophthalmology & Visual Science | 2013

Corneal Epithelial Cell Protective and Wettability-enhancing Properties of Hyaluronic acid + PEG 8000 in an Artificial Tear Product

Stephen R. Davio; Megan E. Cavet; Karen Harrington; Amy Walsh; Zora Marlowe; Brian Glass; Paramita Sarkar

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