e hazard of secondary ocular infections. in acute purulent conditions, steroids may mask infection or enhance existing infection. if signs and symptoms fail to improve after 2 days, the patient should be reevaluated. ( 5.4 ) viral infections: employment of a corticosteroid medication in the treatment of patients with a history of herpes simplex requires great caution. use of ocular steroids may prolong the course and may exacerbate the severity of many viral infections of the eye (including herpes simplex). ( 5.5 ) fungal infections: fungal infections of the cornea are particularly prone to develop coincidentally with long-term local steroid application. fungus invasion must be considered in any persistent corneal ulceration where a steroid has been used or is in use. ( 5.6 ) 5.1 intraocular pressure increase prolonged use of corticosteroids may result in glaucoma with damage to the optic nerve, defects in visual acuity and fields of vision. steroids should be used with caution in the presence of glaucoma. if this product is used for 10 days or longer, intraocular pressure (iop) should be monitored. 5.2 cataracts use of corticosteroids may result in posterior subcapsular cataract formation. 5.3 delayed healing the use of steroids after cataract surgery may delay healing and increase the incidence of bleb formation. in those diseases causing thinning of the cornea or sclera, perforations have been known to occur with the use of topical steroids. the initial prescription and renewal of the medication order beyond 28 days should be made by a physician only after examination of the patient with the aid of magnification, such as slit lamp biomicroscopy, and where appropriate, fluorescein staining. 5.4 bacterial infections prolonged use of corticosteroids may suppress the host response and thus increase the hazard of secondary ocular infections. in acute purulent conditions, steroids may mask infection or enhance existing infection. if signs and symptoms fail to improve after 2 days, the patient should be reevaluated. 5.5 viral infections employment of a corticosteroid medication in the treatment of patients with a history of herpes simplex requires great caution. use of ocular steroids may prolong the course and may exacerbate the severity of many viral infections of the eye (including herpes simplex). 5.6 fungal infections fungal infections of the cornea are particularly prone to develop coincidentally with long-term local steroid application. fungus invasion must be considered in any persistent corneal ulceration where a steroid has been used or is in use. fungal culture should be taken when appropriate. 5.7 topical ophthalmic use only durezol is not indicated for intraocular administration. 5.8 contact lens wear durezol should not be instilled while wearing contact lenses. remove contact lenses prior to instillation of durezol. the preservative in durezol may be absorbed by soft contact lenses. lenses may be reinserted after 10 minutes following administration of durezol.

ndicated.

than 1% of subjects, included application-site discomfort or irritation, corneal pigmentation and striae, episcleritis, eye pruritus, eyelid irritation and crusting, foreign body sensation, increased lacrimation, macular edema, sclera hyperemia, and uveitis. most of these reactions may have been the consequence of the surgical procedure. 6.2 endogenous anterior uveitis a total of 200 subjects participated in the clinical trials for endogenous anterior uveitis, of which 106 were exposed to durezol. the most common adverse reactions of those exposed to durezol occurring in 5% to 10% of subjects included blurred vision, eye irritation, eye pain, headache, increased iop, iritis, limbal and conjunctival hyperemia, punctate keratitis, and uveitis. adverse reactions occurring in 2% to 5% of subjects included anterior chamber flare, corneal edema, dry eye, iridocyclitis, photophobia, and reduced visual acuity.

ince durezol is administered topically with minimal systemic absorption, and difluprednate blood levels were not measured in the reproductive animal studies. however, since use of difluprednate during human pregnancy has not been evaluated and cannot rule out the possibility of harm, durezol should be used during pregnancy only if the potential benefit justifies the potential risk to the embryo or fetus. 8.3 nursing mothers it is not known whether topical ophthalmic administration of corticosteroids could result in sufficient systemic absorption to produce detectable quantities in breast milk. systemically administered corticosteroids appear in human milk and could suppress growth, interfere with endogenous corticosteroid production, or cause other untoward effects. caution should be exercised when durezol is administered to a nursing woman. 8.4 pediatric use durezol was evaluated in a 3-month multicenter, double-masked trial in 79 pediatric patients (39 durezol; 40 prednisolone acetate) 0 to 3 years of age for the treatment of inflammation following cataract surgery. a similar safety profile was observed in pediatric patients comparing durezol to prednisolone acetate ophthalmic suspension, 1%. 8.5 geriatric use no overall differences in safety or effectiveness have been observed between elderly and younger patients.

opically with minimal systemic absorption, and difluprednate blood levels were not measured in the reproductive animal studies. however, since use of difluprednate during human pregnancy has not been evaluated and cannot rule out the possibility of harm, durezol should be used during pregnancy only if the potential benefit justifies the potential risk to the embryo or fetus.

cetylation in vivo to 6α, 9-difluoroprednisolone 17-butyrate (dfb), an active metabolite of difluprednate. clinical pharmacokinetic studies of difluprednate after repeat ocular instillation of 2 drops of difluprednate (0.01% or 0.05%) 4 times per day for 7 days showed that dfb levels in blood were below the quantification limit (50 ng/ml) at all time points for all subjects, indicating the systemic absorption of difluprednate after ocular instillation of durezol is limited.

e molecule and are well known glucocorticosteroid effects. most, if not all of these effects were reversible after drug withdrawal. the noel for the subchronic and chronic toxicity tests were consistent between species and ranged from 1-1.25 mcg/kg/day.

rcent of subjects who were pain free figure 1 percent of subjects with anterior chamber cells clearing (cell count = 0) figure 2 percent of subjects who were pain free 14.2 endogenous anterior uveitis clinical efficacy was evaluated in two randomized, double masked active controlled trials in which patients who presented with endogenous anterior uveitis were treated with either durezol 4 times daily or prednisolone acetate ophthalmic suspension 1%, 8 times daily for 14 days. both studies demonstrated that durezol was equally effective as prednisolone acetate ophthalmic suspension 1% in treating subjects with endogenous anterior uveitis. the results are found in table 1 below. table 1: mean change from baseline in anterior chamber cell grade* abbreviation: ci, confidence interval. *with 5 grades: 0 = 0 cells; 1 = 1 to 10 cells; 2 = 11 to 20 cells; 3 = 21 to 50 cells; and 4 = greater than 50 cells. † adjusted for baseline ac cell grade and study center and based on itt dataset with locf for missing data. study 1 time point durezol n = 57 prednisolone acetate n = 53 difference † (95% ci) baseline 2.6 2.5 0.0 (-0.22, 0.28) day 3 -1.0 -1.0 -0.1 (-0.35, 0.25) day 7 -1.6 -1.5 0.0 (-0.31, 0.25) day 14 -2.0 -1.8 -0.2 (-0.46, 0.10) day 21 -2.2 -1.9 -0.3 (-0.53, 0.01) day 28 -2.2 -2.1 -0.1 (-0.37, 0.18) day 35 -2.1 -2.0 -0.1 (-0.39, 0.20) day 42 -2.1 -2.1 0.0 (-0.27, 0.34) study 2 time point durezol n = 50 prednisolone acetate n = 40 difference † (95% ci) baseline 2.4 2.4 0.0 (-0.21, 0.29) day 3 -0.9 -0.9 0.0 (-0.34, 0.25) day 7 -1.7 -1.6 -0.1 (-0.35, 0.21) day 14 -1.9 -1.8 -0.1 (-0.34, 0.20) day 21 -2.0 -2.0 0.0 (-0.25, 0.28) day 28 -2.0 -2.0 0.0 (-0.21, 0.26) day 35 -2.1 -2.0 -0.1 (-0.32, 0.16) day 42 -2.0 -1.9 -0.1 (-0.36, 0.24)