Twenty-four-hour intraocular pressure control with latanoprost-timolol-fixed
combination versus bimatoprost in patients who switched from timolol.
Author(s): Mesci C, Aydin N, Erbil HH.
Affiliation(s): Ophthalmology Department, Goztepe Training and Research Hospital, Istanbul,
Turkey. cemmesci@ttmail.com
Publication date & source: 2011, J Glaucoma. , 20(8):477-81
PURPOSE: To evaluate bimatoprost versus latanoprost and timolol fixed combination
(LTFC) over the 24-hour diurnal curve in patients who switched from timolol.
METHODS: In this prospective, observer-masked, randomized clinical trial, 64
patients whose intraocular pressures (IOPs) were not effectively controlled with
timolol were enrolled. At pretrial visit IOPs and central corneal thickness were
measured. After the baseline visit, timolol was replaced by bimatoprost or LTFC.
IOPs were recorded at 8 AM, noon, 4 PM, 8 PM, midnight, and 4 AM at baseline,
week 8, and week 16 visits.
RESULTS: At baseline and week 8 visits, there was no significant difference
between the LTFC and bimatoprost group for the mean IOPs at 6 time points in 24
hours, the mean diurnal IOP, and range of diurnal IOP. At week 16, the mean IOP
of the bimatoprost group (15.7±2 mm Hg) at 8 AM and 12 o' clock, midnight, was
statistically significantly lower than that of the LTFC group (16.8±1.5 and
16.9±1.7 mm Hg; P=0.03 and 0.002). A statistically significant difference was not
found between the proportions of patients who had 15% and 20% decrease in mean
diurnal IOP and the mean daytime, nighttime, diurnal IOP reductions of the 2
study groups at weeks 8 and 16 (P>0.05). In the bimatoprost group punctate
epitheliopathy, conjunctival hyperemia, and lid erythema were found to be more
frequent.
CONCLUSIONS: The LTFC and bimatoprost therapies were equally effective in
maintaining IOP at lower levels during the 24-hour period in patients who
switched from timolol therapy. Adverse events were more frequent with bimatoprost
therapy.
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