ith formulations of mupirocin, including mupirocin cream [see adverse reactions ( 6.2 )]. 5.2 eye irritation avoid contact with the eyes. in case of accidental contact, rinse well with water. 5.3 local irritation in the event of a sensitization or severe local irritation from mupirocin cream, usage should be discontinued, and appropriate alternative therapy for the infection instituted. 5.4 clostridium difficile -associated diarrhea clostridium difficile -associated diarrhea (cdad) has been reported with use of nearly all antibacterial agents and may range in severity from mild diarrhea to fatal colitis. treatment with antibacterial agents alters the normal flora of the colon leading to overgrowth of c. difficile . c. difficile produces toxins a and b which contribute to the development of cdad. hypertoxin-producing strains of c. difficile cause increased morbidity and mortality, as these infections can be refractory to antimicrobial therapy and may require colectomy. cdad must be considered in all patients who present with diarrhea following antibacterial drug use. careful medical history is necessary since cdad has been reported to occur over 2 months after the administration of antibacterial agents. if cdad is suspected or confirmed, ongoing antibacterial drug use not directed against c. difficile may need to be discontinued. appropriate fluid and electrolyte management, protein supplementation, antibacterial treatment of c. difficile , and surgical evaluation should be instituted as clinically indicated. 5.5 potential for microbial overgrowth as with other antibacterial products, prolonged use of mupirocin cream may result in overgrowth of nonsusceptible microorganisms, including fungi [see dosage and administration ( 2 )] . 5.6 risk associated with mucosal use mupirocin cream is not formulated for use on mucosal surfaces. a separate formulation, bactroban (mupirocin) nasal ointment, is available for intranasal use.

9 subjects were treated with topical mupirocin cream plus oral placebo. adverse reactions occurred in 28 (8.3%) subjects. the following adverse reactions were reported by at least 1% of subjects in connection with the use of mupirocin cream in clinical trials: headache (1.7%), rash (1.1%), and nausea (1.1%). other adverse reactions which occurred in less than 1% of subjects were: abdominal pain, burning at application site, cellulitis, dermatitis, dizziness, pruritus, secondary wound infection, and ulcerative stomatitis. in a supportive trial in the treatment of secondarily infected eczema, 82 subjects were treated with mupirocin cream. the incidence of adverse reactions was as follows: nausea (4.9%), headache and burning at application site (3.6% each), pruritus (2.4%), and 1 report each of abdominal pain, bleeding secondary to eczema, pain secondary to eczema, hives, dry skin, and rash. 6.2 postmarketing experience in addition to adverse reactions reported from clinical trials, the following reactions have been identified during postmarketing use of mupirocin cream. because they are reported voluntarily from a population of unknown size, estimates of frequency cannot be made. these reactions have been chosen for inclusion due to a combination of their seriousness, frequency of reporting, or potential causal relationship to mupirocin cream. immune system disorders systemic allergic reactions, including anaphylaxis, urticaria, angioedema, and generalized rash [see warnings and precautions ( 5.1 )] .

d subcutaneously to rats and rabbits at doses up to 160 mg per kg per day during organogenesis. this dose is 22 and 43 times, respectively, the human topical dose (approximately 60 mg mupirocin per day) based on calculations of dose divided by the entire body surface area. maternal toxicity was observed (body weight loss/decreased body weight gain and reduced feeding) in both species with no evidence of developmental toxicity in rats. in rabbits, excessive maternal toxicity at the high dose precluded the evaluation of fetal outcomes. there was no developmental toxicity in rabbits at 40 mg per kg per day, 11 times the human topical dose based on calculations of dose divided by the entire body surface area. mupirocin administered subcutaneously to rats in a pre- and postnatal development study (dosed during late gestation through lactation) was associated with reduced offspring viability in the early postnatal period at a dose of 106.7 mg per kg, in the presence of injection site irritation and/or subcutaneous hemorrhaging. this dose is 14 times the human topical dose based on calculations of dose divided by the entire body surface area. the no-observed adverse effect level in this study was 44.2 mg per kg per day, which is 6 times the human topical dose. 8.2 lactation risk summary it is not known whether mupirocin is present in human milk, has effects on the breastfed child, or has effects on milk production. however, breastfeeding is not expected to result in exposure of the child to the drug due to the minimal systemic absorption of mupirocin in humans following topical administration of mupirocin cream [see clinical pharmacology ( 12.3 )] . the developmental and health benefits of breastfeeding should be considered along with the mother’s clinical need for mupirocin cream and any potential adverse effects on the breastfed child from mupirocin cream or from the underlying maternal condition. clinical considerations to minimize oral exposure of the drug to children, a breast and/or nipple being treated with mupirocin cream should be thoroughly washed prior to breastfeeding. 8.4 pediatric use the safety and effectiveness of mupirocin cream have been established in the age-groups of 3 months to 16 years. use of mupirocin cream in these age-groups is supported by evidence from adequate and well-controlled trials of mupirocin cream in adults with additional data from 93 pediatric subjects studied as part of the pivotal trials in adults [see clinical studies ( 14 )] . 8.5 geriatric use in 2 adequate and well-controlled trials, 30 subjects older than 65 years were treated with mupirocin cream. no overall difference in the efficacy or safety of mupirocin cream was observed in this patient population when compared with that observed in younger patients.

abbits at doses up to 160 mg per kg per day during organogenesis. this dose is 22 and 43 times, respectively, the human topical dose (approximately 60 mg mupirocin per day) based on calculations of dose divided by the entire body surface area. maternal toxicity was observed (body weight loss/decreased body weight gain and reduced feeding) in both species with no evidence of developmental toxicity in rats. in rabbits, excessive maternal toxicity at the high dose precluded the evaluation of fetal outcomes. there was no developmental toxicity in rabbits at 40 mg per kg per day, 11 times the human topical dose based on calculations of dose divided by the entire body surface area. mupirocin administered subcutaneously to rats in a pre- and postnatal development study (dosed during late gestation through lactation) was associated with reduced offspring viability in the early postnatal period at a dose of 106.7 mg per kg, in the presence of injection site irritation and/or subcutaneous hemorrhaging. this dose is 14 times the human topical dose based on calculations of dose divided by the entire body surface area. the no-observed adverse effect level in this study was 44.2 mg per kg per day, which is 6 times the human topical dose.

tion. in general, the degree of percutaneous absorption following multiple dosing appears to be minimal in adults and children. the effect of the concurrent application of mupirocin cream with other topical products has not been studied [see dosage and administration ( 2 )] . elimination in a trial conducted in 7 healthy adult male subjects, the elimination half-life after intravenous administration of mupirocin was 20 to 40 minutes for mupirocin and 30 to 80 minutes for monic acid. metabolism: following intravenous or oral administration, mupirocin is rapidly metabolized. the principal metabolite, monic acid, demonstrates no antibacterial activity. excretion: monic acid is predominantly eliminated by renal excretion. 12.4 microbiology mupirocin is an rna synthetase inhibitor antibacterial produced by fermentation using the organism pseudomonas fluorescens . mechanism of action mupirocin inhibits bacterial protein synthesis by reversibly and specifically binding to bacterial isoleucyl-transfer rna (trna) synthetase. mupirocin is bactericidal at concentrations achieved by topical administration. mupirocin is highly protein bound (greater than 97%) and the effect of wound secretions on the minimum inhibitory concentrations (mics) of mupirocin has not been determined. resistance when mupirocin resistance occurs, it results from the production of a modified isoleucyl-trna synthetase, or the acquisition of, by genetic transfer, a plasmid mediating a new isoleucyl-trna synthetase. high-level plasmid-mediated resistance (mic ≥512 mcg/ml) has been reported in increasing numbers of isolates of s. aureus and with higher frequency in coagulase-negative staphylococci. mupirocin resistance occurs with greater frequency in methicillin-resistant than methicillin-susceptible staphylococci. cross resistance due to its mode of action, mupirocin does not demonstrate cross resistance with other classes of antimicrobial agents. antimicrobial activity mupirocin has been shown to be active against susceptible isolates of s. aureus and s. pyogenes , both in vitro and in clinical trials [see indications and usage ( 1 )]. the following in vitro data are available, but their clinical significance is unknown. mupirocin is active against most isolates of staphylococcus epidermidis . susceptibility test methods high-level mupirocin resistance (≥512 mcg/ml) may be determined using standard disk diffusion or broth microdilution tests. 1,2 because of the occurrence of mupirocin resistance in methicillin-resistant s. aureus (mrsa), it is appropriate to test mrsa populations for mupirocin susceptibility prior to the use of mupirocin using a standardized method. 3,4,5

fect of the concurrent application of mupirocin cream with other topical products has not been studied [see dosage and administration ( 2 )] . elimination in a trial conducted in 7 healthy adult male subjects, the elimination half-life after intravenous administration of mupirocin was 20 to 40 minutes for mupirocin and 30 to 80 minutes for monic acid. metabolism: following intravenous or oral administration, mupirocin is rapidly metabolized. the principal metabolite, monic acid, demonstrates no antibacterial activity. excretion: monic acid is predominantly eliminated by renal excretion.

ive performance attributable to mupirocin.

le to mupirocin.

exin (250 mg 4 times daily for subjects greater than 40 kg or 25 mg per kg per day oral suspension in 4 divided doses for subjects less than or equal to 40 kg). clinical efficacy at follow-up (7 to 12 days post-therapy) in the per-protocol populations was 97.7% (43 of 44) for mupirocin cream and 93.9% (46 of 49) for cephalexin.

lips, face, or tongue, or wheezing occur [see warnings and precautions ( 5.1 )] . • if no improvement is seen in 3 to 5 days, contact the healthcare provider. trademarks are the property of their respective owners. manufactured by: glenmark pharmaceuticals limited colvale-bardez, goa 403 513, india manufactured for: glenmark pharmaceuticals inc., usa mahwah, nj 07430 questions? 1 (888) 721-7115 www.glenmarkpharma-us.com march 2020 pharmacist-detach here and give instructions to patient --------------------------------------------------------------------------------------------------------------------------------------------------------------- glenmark-logo