haemophilus influenzae, moraxella catarrhalis*, moraxella lacunata*, pseudomonas aeruginosa*, staphylococcus aureus, staphylococcus epidermidis, staphylococcus hominis*, staphylococcus lugdunensis*, staphylococcus warneri*, streptococcus mitis group , streptococcus oralis, streptococcus pneumoniae, streptococcus salivarius* *efficacy for this organism was studied in fewer than 10 infections. ( 1 )

herapy with besivance.

-fda-1088 or www.fda.gov/medwatch .

, the mean c max in the rat dams was approximately 20 mcg/ml, approximately 46,500 times the mean plasma concentrations measured in humans at the recommended human ophthalmic dose (rhod). the no observed adverse effect level (noael) for this embryofetal development study was 100 mg/kg/day (c max , 5 mcg/ml, approximately 11,600 times the mean plasma concentrations measured in humans at the rhod). in a prenatal and postnatal development study in rats, the noaels for both fetal/neonate and maternal toxicity were 100 mg/kg/day. at 1,000 mg/kg/day, pups weighed significantly less than controls and had a reduced neonatal survival rate. attainment of developmental landmarks and sexual maturation was delayed, although surviving pups from this dose group that were reared to maturity did not demonstrate deficits in behavior, including activity, learning and memory, and their reproductive capacity appeared normal. 8.2 lactation risk summary there are no data on the presence of besivance in human milk, the effects on the breastfed infant, or the effects on milk production. however, systemic exposure to besifloxacin following topical ocular administration is low [see clinical pharmacology (12.3) ] , and it is not known whether measurable levels of besifloxacin would be present in maternal milk following topical ocular administration. the developmental and health benefits of breastfeeding should be considered, along with the mother’s clinical need for besivance, and any potential adverse effects on the breastfed infant from besivance. 8.4 pediatric use the safety and effectiveness of besivance in infants below one year of age have not been established. the efficacy of besivance in treating bacterial conjunctivitis in pediatric patients one year or older has been demonstrated in controlled clinical trials [see clinical studies (14)]. there is no evidence that the ophthalmic administration of quinolones has any effect on weight-bearing joints, even though systemic administration of some quinolones has been shown to cause arthropathy in immature animals. 8.5 geriatric use no overall differences in safety and effectiveness have been observed between elderly and younger patients.

ms was approximately 20 mcg/ml, approximately 46,500 times the mean plasma concentrations measured in humans at the recommended human ophthalmic dose (rhod). the no observed adverse effect level (noael) for this embryofetal development study was 100 mg/kg/day (c max , 5 mcg/ml, approximately 11,600 times the mean plasma concentrations measured in humans at the rhod). in a prenatal and postnatal development study in rats, the noaels for both fetal/neonate and maternal toxicity were 100 mg/kg/day. at 1,000 mg/kg/day, pups weighed significantly less than controls and had a reduced neonatal survival rate. attainment of developmental landmarks and sexual maturation was delayed, although surviving pups from this dose group that were reared to maturity did not demonstrate deficits in behavior, including activity, learning and memory, and their reproductive capacity appeared normal.

e iv is an essential enzyme required for partitioning of the chromosomal dna during bacterial cell division. besifloxacin is bactericidal with minimum bactericidal concentrations (mbcs) generally within one dilution of the minimum inhibitory concentrations (mics). the mechanism of action of fluoroquinolones, including besifloxacin, is different from that of aminoglycoside, macrolide, and β -lactam antibiotics. therefore, besifloxacin may be active against pathogens that are resistant to these antibiotics and these antibiotics may be active against pathogens that are resistant to besifloxacin. in vitro studies demonstrated cross-resistance between besifloxacin and some fluoroquinolones. in vitro resistance to besifloxacin develops via multiple-step mutations and occurs at a general frequency of <3.3 x 10 -10 for staphylococcus aureus and <7 x 10 -10 for streptococcus pneumoniae . besifloxacin has been shown to be active against most isolates of the following bacteria both in vitro and in conjunctival infections treated in clinical trials [see indications and usage (1) ]: aerococcus viridans* cdc coryneform group g corynebacterium pseudodiphtheriticum* corynebacterium striatum* haemophilus influenzae moraxella catarrhalis* moraxella lacunata* pseudomonas aeruginosa* staphylococcus aureus staphylococcus epidermidis staphylococcus hominis* staphylococcus lugdunensis* staphylococcus warneri* streptococcus mitis group streptococcus oralis streptococcus pneumoniae streptococcus salivarius* *efficacy for this organism was studied in fewer than 10 infections.

cin did not impair the fertility of male or female rats at oral doses of up to 500 mg/kg/day. this dose is approximately 26,500 times higher than the mean plasma concentration measured in humans at the recommended human ophthalmic dose.

tility of male or female rats at oral doses of up to 500 mg/kg/day. this dose is approximately 26,500 times higher than the mean plasma concentration measured in humans at the recommended human ophthalmic dose.