were 2 months to less than 2 years of age, 55 % of patients were 2 to less than 12 years of age, 11 % of patients were 12 to less than 18 years of age, and 31 % of patients were 18 years of age or older. adverse reactions (rosacea and seborrheic dermatitis) were reported in 1 adult patient treated with xepi.

riage in clinically recognized pregnancies is 2% to 4% and 15% to 20%, respectively. 8.2 lactation risk summary no data are available regarding the presence of ozenoxacin in human milk, and the effects of ozenoxacin on the breastfed infant or on milk production. however, breastfeeding is not expected to result in exposure of the child to ozenoxacin due to the negligible systemic absorption of ozenoxacin in humans following topical administration of xepi. the developmental and health benefits of breastfeeding should be considered along with the mother's clinical need for xepi and any potential adverse effects on the breast-fed child from xepi or from the underlying maternal condition. 8.4 pediatric use the safety and effectiveness of xepi in the treatment of impetigo have been established in pediatric patients 2 months to 17 years of age. use of xepi in pediatric patients (2 months to 17 years of age) is supported by evidence from adequate and well-controlled studies of xepi in which 251 pediatric patients received at least one dose of xepi. the median age of the patients enrolled in the clinical trials was 10 years; 3 % of patients were 2 months to less than 2 years of age, 55 % of patients were 2 to less than 12 years of age, 11 % of patients were 12 to less than 18 years of age, and 31 % of patients were 18 years of age or older. in these studies, the maximum dose applied was approximately 0.5 g of xepi applied twice daily for up to 5 days (i.e., up to 10 applications total) [see clinical studies (14) ] . the safety profile of xepi in pediatric patients 2 months and older was similar to that of adults [see adverse reactions (6.1) ] . the safety and effectiveness of xepi in pediatric patients younger than 2 months of age have not been established [see clinical studies (14) ] . 8.5 geriatric use clinical studies of xepi did not include sufficient numbers of subjects aged 65 and older to determine whether they respond differently from younger subjects. other reported clinical experience has not identified differences in responses between the elderly and younger patients.

pregnancies is 2% to 4% and 15% to 20%, respectively.

of xepi in pediatric patients younger than 2 months of age have not been established [see clinical studies (14) ] .

tection (0.489 ng/ml) in 2 subjects. distribution plasma protein binding of [ 14 c]-ozenoxacin was moderate (~80 to 85%) and did not appear to be dependent on concentration. since negligible systemic absorption was observed in clinical studies, tissue distribution has not been investigated in humans. elimination metabolism: ozenoxacin was not metabolized in the presence of fresh human skin discs and was minimally metabolized in human hepatocytes. excretion: studies have not been investigated in humans due to the negligible systemic absorption observed in clinical studies. 12.4 microbiology mechanism of action ozenoxacin is a quinolone antimicrobial drug. the mechanism of action involves the inhibition of bacterial dna replication enzymes, dna gyrase a and topoisomerase iv. ozenoxacin has been shown to be bactericidal against s. aureus and s. pyogenes organisms. resistance the mechanism of quinolone resistance can arise through mutations of one or more of the genes that encode dna gyrase or topoisomerase iv. resistant organisms will typically carry a combination of mutations within gyra and parc subunits. overall the frequency of resistant mutants selected by ozenoxacin is ≤10 -10 . interaction with other antimicrobials ozenoxacin has been tested in combination with 17 other commonly used antimicrobial agents against s. aureus and s.pyogenes . antagonism interactions with ozenoxacin were observed with ciprofloxacin against s. aureus . antimicrobial activity ozenoxacin has been shown to be active against most isolates of the following microorganisms, both in vitro and in clinical infections [see indications and usage (1) ]: gram-positive bacteria staphylococcus aureus (including methicillin-resistant isolates) streptococcus pyogenes

inimally metabolized in human hepatocytes. excretion: studies have not been investigated in humans due to the negligible systemic absorption observed in clinical studies.

issue warmth, and pain; and erythema/inflammation, tissue edema, and itching assessed as less than mild in trial 1; and absence of blistering, exudates/pus, crusting, and itching/pain, and mild or improved erythema/inflammation in trial 2. table 2 below presents the results for clinical response at the end of therapy. table 2 clinical response at end of therapy in trial 1 and trial 2 in all randomized subjects trial 1 trial 2 xepi placebo xepi placebo (n = 155) n (%) (n = 156) n (%) (n = 206) n (%) (n = 206) n (%) a the success rates for ozenoxacin were significantly different than placebo in study 1 and study 2 (p = 0.002 and p = 0.001). clinical success 54 (34.8) 30 (19.2) 112 (54.4) 78 (37.9) clinical failure 98 (63.2) 120 (76.9) 91 (44.2) 121 (58.7) unable to determine 3 (1.9) 6 (3.8) 3 (1.5) 7 (3.4) the most commonly identified bacteria were s. aureus and s. pyogenes . table 3 below presents the results for clinical success at end of therapy in subjects with s.aureus or s.pyogenes at baseline. table 3 clinical success at end of therapy in trial 1 and trial 2 in subjects with s. aureus or s. pyogenes trial 1 trial 2 xepi placebo xepi placebo clinical success n/n (%) n/n (%) n/n (%) n/n (%) s. aureus 35/93 (37.6) 16/98 (16.3) 66/115 (57.4) 36/108 (33.3) s. pyogenes 29/73 (39.7) 7/67 (10.4) 15/19 (78.9) 8/20 (40.0)