medical attention immediately and consider a dermatological evaluation.

ne year of age or older: 0.9 mg/kg given as an intravenous infusion once daily. ( 2.3 ) 2.1 patient selection start nulibry if the patient has a diagnosis or presumptive diagnosis of mocd type a. in patients with a presumptive diagnosis of mocd type a, confirm the diagnosis of mocd type a immediately after initiation of nulibry treatment. in such patients, discontinue nulibry if the mocd type a diagnosis is not confirmed by genetic testing. 2.2 important administration information nulibry is intended for administration by a healthcare provider. if deemed appropriate by a healthcare provider, nulibry may be administered at home by the patient's caregiver. if nulibry can be administered by a caregiver/patient, advise them to read the detailed instructions on the preparation, administration, storage, and disposal of nulibry for caregivers [see instructions for use ]. nulibry is for intravenous infusion only. administer with non-dehp tubing with a 0.2 micron filter. do not mix nulibry with other drugs (note nulibry is reconstituted with sterile water for injection, usp). do not administer as an infusion with other drugs. nulibry is given through an infusion pump at a rate of 1.5 ml per minute. dose volumes below 2 ml may require syringe administration through slow intravenous push. administration of nulibry must be completed within 4 hours of reconstitution [see dosage and administration ( 2.5 )] . 2.3 recommended dosage and administration recommended dosage and administration in patients less than one year of age (by gestational age) the recommended dosage regimen of nulibry in patients less than one year of age (by gestational age) is based on actual body weight as shown in table 1 . table 1 recommended initial dosage and titration schedule of nulibry for patients less than one year of age by gestational age titration schedule preterm neonates (gestational age less than 37 weeks) term neonates (gestational age 37 weeks and above) initial dosage 0.4 mg/kg once daily 0.55 mg/kg once daily dosage at month 1 0.7 mg/kg once daily 0.75 mg/kg once daily dosage at month 3 0.9 mg/kg once daily 0.9 mg/kg once daily recommended dosage and administration in patients one year of age or older for patients one year of age or older, the recommended dosage of nulibry is 0.9 mg/kg (based on actual body weight) administered as an intravenous infusion once daily. recommendations for a missed dose if a nulibry dose is missed, administer the missed dose as soon as possible. administer the next scheduled dose at least 6 hours after the administration of the missed dose. 2.4 preparation and administration instructions nulibry must be reconstituted prior to use. use aseptic technique during preparation and follow these instructions: determine the total dose, number of vials needed, and total reconstituted dose volume based on the patient's weight and prescribed dose. remove the required number of vials from the freezer to allow them to reach room temperature (by hand warming for 3 to 5 minutes or exposing to ambient air for approximately 30 minutes). reconstitute each required nulibry vial with 5 ml of sterile water for injection, usp. gently swirl the vial continuously until the powder is completely dissolved. do not shake. after reconstitution, the final concentration of nulibry reconstituted solution is 9.5 mg/5 ml (1.9 mg/ml). parenteral drug products should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit. reconstituted nulibry is a clear and colorless to pale yellow solution. do not use if there are particles present or if the solution is discolored. administer the total reconstituted dose. 2.5 storage of reconstituted solution reconstituted nulibry may be stored at room temperature [15°c to 25°c (59°f to 77°f)] or refrigerated [2°c to 8°c (36°f to 46°f)] for up to 4 hours including infusion time. if reconstituted nulibry is refrigerated, allow it to come to room temperature (by hand warming for 3 to 5 minutes or exposing to ambient air for approximately 30 minutes) before administration. do not heat. do not re-freeze nulibry after reconstitution. do not shake. discard all unused reconstituted nulibry solution 4 hours after reconstitution.

e biologic activity as nulibry). of these 37 patients/healthy adults, 13 were pediatric patients with mocd type a in studies 1, 2, and 3 [see clinical studies ( 14 )] , 6 were pediatric patients with presumptive mocd type a but who were later confirmed to not have mocd type a, and 18 were healthy adults (without mocd type a) in a phase 1 study. adverse reactions assessment of adverse reactions for nulibry is based on data from two open-label, single-arm studies, study 1 (n=8) and study 2 (n=1), in patients with a confirmed diagnosis of mocd type a (8 of the 9 patients were previously treated with rcpmp). in these studies, patients received a daily intravenous infusion of nulibry. the median exposure to nulibry was 4.3 years and ranged from 8 days to 5.6 years [see clinical studies ( 14 )]. in these studies, 44% of patients were males and 56% were females, 67% were white and 33% were asian. the mean age was 14 days and ranged from 1 day to 69 days at time of first infusion. table 2 presents the most common adverse reactions that occurred in nulibry-treated patients in studies 1 and 2. table 2 common adverse reactions reported in two or more nulibry-treated patients with mocd type a (studies 1 and 2) abbreviations: mocd = molybdenum cofactor deficiency 1 catheter-related complications included complication associated with device, catheter site abscess, catheter site discharge, catheter site extravasation, catheter site pain, catheter site infection, catheter site inflammation, device dislocation, device leakage, device occlusion, and vascular device infection. adverse reactions nulibry-treated patients (n=9) n (%) catheter-related complications 1 8 (89%) pyrexia 7 (78%) viral infection 5 (56%) pneumonia 4 (44%) otitis media 4 (44%) vomiting 4 (44%) cough/sneezing 4 (44%) upper viral respiratory infection 3 (33%) gastroenteritis 3 (33%) diarrhea 3 (33%) bacteremia 3 (33%) abdominal pain 2 (22%) influenza 2 (22%) lower respiratory tract infection 2 (22%) viral tonsillitis 2 (22%) oropharyngeal pain 2 (22%) rash maculo-papular 2 (22%) anemia 2 (22%) eye swelling 2 (22%) seizure 2 (22%) agitation 2 (22%) safety data are also available from 10 patients with mocd type a who received rcpmp in study 3 (an observational study) [see clinical studies ( 14 )]. the median time on rcpmp treatment was 1.5 years and ranged from 6 days to 4.4 years. in study 3, the patient population was evenly distributed between males and females with a mean age of 18 days (range 1, 69) at time of first infusion, 70% were white, and 30% were asian. in study 3, one patient died of necrotizing enterocolitis. adverse reactions for the rcpmp-treated patients were similar to the nulibry-treated patients, except for the following additional adverse reactions that were reported in more than one patient: sepsis, oral candidiasis, varicella, fungal skin infection, and eczema.

ong with the mother's clinical need for nulibry and any potential adverse effects on the breastfed infant from nulibry or from the underlying maternal condition. 8.4 pediatric use safety and effectiveness of nulibry for the treatment of mocd type a have been established in pediatric patients starting from birth. use of nulibry for this indication is supported by evidence from two open-label studies (studies 1 and 2) and one observational study (study 3), in which 13 pediatric patients aged birth to 6 years of age were treated with nulibry or rcpmp. pediatric use information is discussed throughout the labeling. animal studies have identified that nulibry has phototoxic potential. advise nulibry-treated patients or their caregivers to avoid patient exposure to direct sunlight and artificial uv light exposure (i.e., uva or uvb phototherapy) and adopt precautionary measures [see warnings and precautions ( 5.1 ) and nonclinical toxicology ( 13.2 )]. 8.5 geriatric use mocd type a is largely a disease of pediatric patients. clinical studies of nulibry did not include patients 65 years of age and older. 8.6 adult use the safety and effectiveness of nulibry for the treatment of adults with mocd type a have been established. use of nulibry in adults for this indication is based on an adequate and well- controlled clinical investigation in pediatric patients [see clinical studies ( 14 )].

extent. 12.3 pharmacokinetics the pharmacokinetics of fosdenopterin in healthy adult subjects following a single intravenous nulibry infusion are summarized in table 3 . the area under the plasma concentration-time curve (auc) and the maximum plasma concentration (c max ) of fosdenopterin increased in an approximately proportional manner with increasing doses. table 3 mean (sd) pharmacokinetic parameters following a single intravenous dose of fosdenopterin in healthy subjects 1 0.075 mg/kg, 0.24 mg/kg, and 0.68 mg/kg doses are 0.08, 0.27, and 0.76 times the recommended maximum dose, respectively. parameter 0.075 mg/kg 1 0.24 mg/kg 1 0.68 mg/kg 1 c max (ng/ml) 285 (57) 873 (99) 2800 (567) auc 0-inf (ng*h/ml) 523 (75) 1790 (213) 5960 (1820) distribution the volume of distribution (v d ) of fosdenopterin was approximately 300 ml/kg. the plasma protein binding of fosdenopterin ranged from 6 to 12%. elimination the mean total body clearance (cl) of fosdenopterin ranged from 167 to 195 ml/h/kg. the mean half-life of fosdenopterin ranged from 1.2 to 1.7 hours. metabolism fosdenopterin is predominantly metabolized through nonenzymatic degradation processes to compound z, an inactive oxidation product of endogenous cpmp. excretion renal clearance of fosdenopterin accounts for approximately 40% of total body clearance. specific populations the effect of renal and hepatic impairment on the pharmacokinetics of fosdenopterin is unknown. pediatric patients pharmacokinetic properties of fosdenopterin in pediatric mocd type a patients are similar to healthy adult subjects. drug interaction studies in vitro studies cytochrome p450 (cyp) enzymes : fosdenopterin does not inhibit cyp1a2, cyp2b6, cyp2c8, cyp2c9, cyp2c19, cyp2d6, or cyp3a4/5. fosdenopterin does not induce cyp1a2, cyp2b6, or cyp3a4. transporter systems : fosdenopterin is a weak inhibitor of mate2-k and oat1, but does not inhibit p-gp, bcrp, oatp1b1, oatp1b3, oct2, oat3, and mate1. fosdenopterin is a weak substrate for mate1, but is not a substrate of p-gp, bcrp, oatp1b1, oatp1b3, oct2, oat1, oat3, or mate2-k.

mean half-life of fosdenopterin ranged from 1.2 to 1.7 hours. metabolism fosdenopterin is predominantly metabolized through nonenzymatic degradation processes to compound z, an inactive oxidation product of endogenous cpmp. excretion renal clearance of fosdenopterin accounts for approximately 40% of total body clearance. specific populations the effect of renal and hepatic impairment on the pharmacokinetics of fosdenopterin is unknown. pediatric patients pharmacokinetic properties of fosdenopterin in pediatric mocd type a patients are similar to healthy adult subjects. drug interaction studies in vitro studies cytochrome p450 (cyp) enzymes : fosdenopterin does not inhibit cyp1a2, cyp2b6, cyp2c8, cyp2c9, cyp2c19, cyp2d6, or cyp3a4/5. fosdenopterin does not induce cyp1a2, cyp2b6, or cyp3a4. transporter systems : fosdenopterin is a weak inhibitor of mate2-k and oat1, but does not inhibit p-gp, bcrp, oatp1b1, oatp1b3, oct2, oat3, and mate1. fosdenopterin is a weak substrate for mate1, but is not a substrate of p-gp, bcrp, oatp1b1, oatp1b3, oct2, oat1, oat3, or mate2-k.

ngs and precautions ( 5.1 )].

tient (i.e., 36 weeks). the initial dosage was then incrementally escalated up to a maximum dosage of 0.98 mg/kg administered once daily as an intravenous infusion (1.1 times the maximum approved recommended dosage) [see dosage and administration ( 2.3 )]. study 3 study 3 was a retrospective, observational study that included 10 patients with a confirmed diagnosis of mocd type a who received rcpmp. six of these 10 patients were later enrolled in study 1 to receive treatment with nulibry. efficacy results the efficacy of nulibry and rcpmp were assessed in a combined analysis of the 13 patients with genetically confirmed mocd type a from study 1 (n=8), study 2 (n=1), and study 3 (n=4) who received substrate replacement therapy with nulibry or rcpmp. of the 13 treated patients included in the combined analysis, 54% were male, 77% were white and 23% were asian; the median gestational age was 39 weeks (range 35 to 41 weeks). of these 13 treated patients, the age at first dose was ≤ 14 days for 10 patients (with 5 patients initiating treatment at 1 day of age) and ≥ 32 days and < 69 days for the remaining 3 patients. overall survival efficacy was assessed by comparing overall survival in pediatric patients treated with nulibry or rcpmp (n=13) with an untreated natural history cohort of pediatric patients with genetically confirmed mocd type a who were genotype-matched to the treated patients (n=18). patients treated with nulibry or rcpmp had an improvement in overall survival compared to the untreated, genotype-matched, historical control group ( table 4 and figure 1 ). results were similar when comparing treated patients with all patients in the untreated natural history cohort with genetically confirmed mocd type a (n=37, includes the 18 genotype-matched untreated patients as well as 19 additional untreated patients who were not genotype-matched). table 4 overall survival in patients with mocd type a treated with nulibry or rcpmp versus genotype-matched untreated patients in historical control abbreviations: ci=confidence interval; ne=not estimable; rcpmp=recombinant escherichia coli -derived cpmp. a quartile estimates from product-limit (kaplan-meier) method, with associated log-log confidence intervals. b based on the area under the survival curves up to 1 year of follow-up. c based on the area under the survival curves up to 3 years of follow-up. d based on cox proportional hazards model regressing survival status on an indicator variable denoting treatment status. the 95% cis are based on the modified score test statistic under the cox model. the hazard ratio represents the risk of death in the treated patients compared to the untreated historical control patients. nulibry (or rcpmp) (n=13) untreated genotype-matched historical control (n=18) treatment difference (95% ci) number of deaths (%) 2 (15%) 12 (67%) 50th percentile (median) survival time in months (95% ci) a ne (16, ne) months 48 (10, 99) months kaplan meier survival probability (95% ci) 1 year 92% (57%, 99%) 67% (40%, 83%) 3 years 84% (49%, 96%) 55% (30%, 74%) mean survival time (months) at 1 year b (95% ci) 11 (9, 13) months 10 (8, 12) months 1 (-1, 4) months at 3 years c (95% ci) 32 (26, 37) months 24 (17, 31) months 8 (-1, 16) months hazard ratio for risk of death (95% ci) d 0.18 (0.04, 0.72) figure 1 kaplan meier curve for overall survival in patients with mocd type a treated with nulibry or rcpmp versus genotype-matched untreated patients in historical control abbreviations: rcpmp=recombinant escherichia coli -derived cpmp figure 1 mocd biomarker results treatment with nulibry resulted in a reduction in urine concentrations of ssc in patients with mocd type a and the reduction was sustained with long-term treatment over 48 months. the baseline level of urinary ssc normalized to creatinine was characterized in one patient (study 2) with a value of 89.8 μmol/mmol. following treatment with nulibry in studies 1 and 2 (n=9), the mean ± sd levels of urinary ssc normalized to creatinine ranged from 11 (±8.5) to 7 (±2.4) μmol/mmol from month 3 to month 48.

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