en age 5 years and older. the safety and effectiveness of the use of ipratropium bromide nasal solution 0.06% (nasal spray) beyond three weeks in patients with seasonal allergic rhinitis have not been established. initial pump priming requires seven sprays of the pump. if used regularly as recommended, no further priming is required. if not used for more than 24 hours, the pump will require two sprays, or if not used for more than seven days, the pump will require seven sprays to reprime. avoid spraying into eyes.

greater in the ipratropium bromide group and higher in the ipratropium bromide group than in the vehicle group. ipratropium bromide nasal solution 0.06% (nasal spray) vehicle control no. of patients 352 351 epistaxis epistaxis reported by 5.4% of ipratropium bromide patients and 1.4% of vehicle patients, blood-tinged nasal mucus by 2.8% of ipratropium bromide patients and 0.9% of vehicle patients. 8.2% 2.3% nasal dryness 4.8% 2.8% dry mouth/throat 1.4% 0.3% nasal congestion 1.1% 0.0% ipratropium bromide nasal solution 0.06% (nasal spray) was well tolerated by most patients. the most frequently reported adverse events were transient episodes of nasal dryness or epistaxis. the majority of these adverse events (96%) were mild or moderate in nature, none was considered serious, and none resulted in hospitalization. no patient required treatment for nasal dryness, and only three patients (<1%) required treatment for epistaxis, which consisted of local application of pressure or a moisturizing agent (e.g., petroleum jelly). no patient receiving ipratropium bromide nasal solution 0.06% (nasal spray) was discontinued from the trial due to either nasal dryness or bleeding. adverse events reported by less than 1% of the patients receiving ipratropium bromide nasal solution 0.06% (nasal spray) during the controlled clinical trials that are potentially related to ipratropium bromide’s local effects or systemic anticholinergic effects include: taste perversion, nasal burning, conjunctivitis, coughing, dizziness, hoarseness, palpitation, pharyngitis, tachycardia, thirst, tinnitus and blurred vision. no controlled trial was conducted to address the relative incidence of adverse events for three times daily versus four times daily therapy. nasal adverse events seen in the clinical trial with seasonal allergic rhinitis (sar) patients (see table 2 ) were similar to those seen in the common cold trials. additional events were reported at a higher rate in the sar trial due in part to the longer duration of the trial and the inclusion of upper respiratory tract infection (uri) as an adverse event. in common cold trials, uri was the disease under study and not an adverse event. table 2 % of patients with sar reporting events this table includes adverse events for which the incidence was 1% or greater in ipratropium bromide group and higher in the ipratropium bromide group than in the vehicle group. ipratropium bromide nasal solution 0.06% (nasal spray) vehicle control no. of patients 218 211 epistaxis epistaxis reported by 3.7% of ipratropium bromide patients and 2.4% of vehicle patients, blood-tinged nasal mucus by 2.3% of ipratropium bromide patients and 1.9% of vehicle patients. 6.0% 3.3% pharyngitis 5.0% 3.8% uri 5.0% 3.3% nasal dryness 4.6% 0.9% headache 4.1% 0.5% dry mouth/throat 4.1% 0.0% taste perversion 3.7% 1.4% sinusitis 2.8% 2.8% pain 1.8% 0.9% diarrhea 1.8% 0.5% there were no reports of allergic-type reactions in the controlled clinical common cold and sar trials. to report suspected adverse reactions, contact bausch & lomb incorporated at 1-800-321-4576 or fda at 1-800-fda-1088 or www.fda.gov/medwatch .

oximately 1,100 times the mrdid in adults on a mg/m 2 basis), embryotoxicity was observed as increased resorption. this effect is not considered relevant to human use due to the large doses at which it was observed and the difference in route of administration.

ray) at a dose of two sprays (84 mcg) per nostril four times a day (total dose 672 mcg/day) for three weeks in pediatric seasonal allergic rhinitis patients down to 5 years is based upon the safety demonstrated in the pediatric common cold trials and the trial in adult and adolescent patients 12 to 75 years of age with seasonal allergic rhinitis. the effectiveness of ipratropium bromide nasal solution 0.06% (nasal spray) for the treatment of rhinorrhea associated with the common cold and seasonal allergic rhinitis in this pediatric age group is based on extrapolation of the demonstrated efficacy of ipratropium bromide nasal solution 0.06% (nasal spray) in adolescents and adults with the conditions and the likelihood that the disease course, pathophysiology, and the drug’s effects are substantially similar to that of adults. the recommended dose for common cold for the pediatric population is based on cross-study comparisons of the efficacy of ipratropium bromide nasal solution 0.06% (nasal spray) in adult and pediatric patients and on its safety profile in both adults and pediatric common cold patients. the recommended dose for seasonal allergic rhinitis for the pediatric population down to 5 years is based upon the efficacy and safety of ipratropium bromide nasal solution 0.06% (nasal spray) in adults and adolescents 12 years of age and above with seasonal allergic rhinitis and the safety profile of this dose in both adult and pediatric common cold patients. the safety and effectiveness of ipratropium bromide nasal solution 0.06% (nasal spray) in pediatric patients under 5 years of age have not been established.

bed from the nasal mucosa of normal volunteers, induced-cold adult volunteers, naturally acquired common cold pediatric patients, or perennial rhinitis adult patients. distribution : ipratropium bromide is minimally bound (0 to 9% in vitro) to plasma albumin and α 1 -acid glycoprotein. its blood/plasma concentration ratio was estimated to be about 0.89. studies in rats have shown that ipratropium bromide does not penetrate the blood-brain barrier. metabolism : ipratropium bromide is partially metabolized to ester hydrolysis products, tropic acid, and tropane. these metabolites appear to be inactive based on in vitroreceptor affinity studies using rat brain tissue homogenates. elimination : after intravenous administration of 2 mg ipratropium bromide to 10 healthy volunteers, the terminal half-life of ipratropium bromide was approximately 1.6 hours. the total body clearance and renal clearance were estimated to be 2,505 and 1,019 ml/min, respectively. the amount of the total dose excreted unchanged in the urine (ae) within 24 hours was approximately one-half of the administered dose. pediatrics : following administration of 84 mcg of ipratropium bromide per nostril three times a day in patients 5-18 years old (n=42) with a naturally acquired common cold, the mean amount of the total dose excreted unchanged in the urine of 7.8% was comparable to 84 mcg per nostril four times a day in an adult induced common cold population (n=22) of 7.3 to 8.1%. plasma ipratropium concentrations were relatively low (ranging from undetectable up to 0.62 ng/ml). no correlation of the amount of the total dose excreted unchanged in the urine (ae) with age or gender was observed in the pediatric population. special populations : gender does not appear to influence the absorption or excretion of nasally administered ipratropium bromide. the pharmacokinetics of ipratropium bromide have not been studied in patients with hepatic or renal insufficiency or in the elderly. drug-drug interactions : no specific pharmacokinetic studies were conducted to evaluate potential drug-drug interactions. pharmacodynamics: in two single dose trials (n=17), doses up to 336 mcg of ipratropium bromide did not significantly affect pupillary diameter, heart rate, or systolic/diastolic blood pressure. similarly, ipratropium bromide nasal solution 0.06% (nasal spray) in adult patients (n=22) with induced-colds, (84 mcg/nostril four times a day) and in pediatric patients (n=45) with naturally acquired common cold (84 mcg/nostril three times a day) had no significant effects on pupillary diameter, heart rate, or systolic/diastolic blood pressure. controlled clinical trials demonstrated that intranasal fluorocarbon-propelled ipratropium bromide does not alter physiologic nasal functions (e.g., sense of smell, ciliary beat frequency, mucociliary clearance, or the air conditioning capacity of the nose). clinical trials: the clinical trials for ipratropium bromide nasal solution 0.06% (nasal spray) were conducted in patients with rhinorrhea associated with naturally occurring common colds. in two controlled four day comparisons of ipratropium bromide nasal solution 0.06% (nasal spray) (84 mcg per nostril, administered three or four times daily; n=352) with its vehicle (n=351), there was a statistically significant reduction of rhinorrhea, as measured by both nasal discharge weight and the patients’ subjective assessment of severity of rhinorrhea using a visual analog scale. these significant differences were evident within one hour following dosing. there was no effect of ipratropium bromide nasal solution 0.06% (nasal spray) on degree of nasal congestion or sneezing. the response to ipratropium bromide nasal solution 0.06% (nasal spray) did not appear to be affected by age or gender. no controlled clinical trials directly compared the efficacy of three times daily versus four times daily treatment. one clinical trial was conducted with ipratropium bromide nasal solution 0.06% (nasal spray), administered four times daily for three weeks, in 218 patients with rhinorrhea associated with seasonal allergic rhinitis (sar), compared to its vehicle in 211 patients. patients in this trial were adults and adolescents 12 years of age and above. ipratropium bromide nasal solution 0.06% (nasal spray) was significantly more effective in reducing the severity and duration of rhinorrhea over the three weeks of the study, as measured by daily patient symptom scores. there was no difference between treatment groups in the effect on nasal congestion, sneezing or itching eyes.

fe of ipratropium bromide was approximately 1.6 hours. the total body clearance and renal clearance were estimated to be 2,505 and 1,019 ml/min, respectively. the amount of the total dose excreted unchanged in the urine (ae) within 24 hours was approximately one-half of the administered dose. pediatrics : following administration of 84 mcg of ipratropium bromide per nostril three times a day in patients 5-18 years old (n=42) with a naturally acquired common cold, the mean amount of the total dose excreted unchanged in the urine of 7.8% was comparable to 84 mcg per nostril four times a day in an adult induced common cold population (n=22) of 7.3 to 8.1%. plasma ipratropium concentrations were relatively low (ranging from undetectable up to 0.62 ng/ml). no correlation of the amount of the total dose excreted unchanged in the urine (ae) with age or gender was observed in the pediatric population. special populations : gender does not appear to influence the absorption or excretion of nasally administered ipratropium bromide. the pharmacokinetics of ipratropium bromide have not been studied in patients with hepatic or renal insufficiency or in the elderly. drug-drug interactions : no specific pharmacokinetic studies were conducted to evaluate potential drug-drug interactions. pharmacodynamics: in two single dose trials (n=17), doses up to 336 mcg of ipratropium bromide did not significantly affect pupillary diameter, heart rate, or systolic/diastolic blood pressure. similarly, ipratropium bromide nasal solution 0.06% (nasal spray) in adult patients (n=22) with induced-colds, (84 mcg/nostril four times a day) and in pediatric patients (n=45) with naturally acquired common cold (84 mcg/nostril three times a day) had no significant effects on pupillary diameter, heart rate, or systolic/diastolic blood pressure. controlled clinical trials demonstrated that intranasal fluorocarbon-propelled ipratropium bromide does not alter physiologic nasal functions (e.g., sense of smell, ciliary beat frequency, mucociliary clearance, or the air conditioning capacity of the nose).

a decrease in the conception rate.

es daily treatment. one clinical trial was conducted with ipratropium bromide nasal solution 0.06% (nasal spray), administered four times daily for three weeks, in 218 patients with rhinorrhea associated with seasonal allergic rhinitis (sar), compared to its vehicle in 211 patients. patients in this trial were adults and adolescents 12 years of age and above. ipratropium bromide nasal solution 0.06% (nasal spray) was significantly more effective in reducing the severity and duration of rhinorrhea over the three weeks of the study, as measured by daily patient symptom scores. there was no difference between treatment groups in the effect on nasal congestion, sneezing or itching eyes.

f ipratropium bromide nasal solution 0.06% (nasal spray), patients should be cautioned about engaging in activities requiring balance and visual acuity such as driving a car or operating appliances, machinery, etc.