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FDA Drug information

VIDAZA

Read time: 7 mins
Marketing start date: 23 Dec 2024

Summary of product characteristics


Adverse Reactions

6 ADVERSE REACTIONS The following adverse reactions are described in other labeling sections: o Anemia, Neutropenia and Thrombocytopenia [see Warnings and Precautions ( 5.2 )] o Hepatotoxicity in Patients with Severe Pre-existing Hepatic Impairment [see Warnings and Precautions ( 5.3 )] o Renal Toxicity [see Warnings and Precautions ( 5.4 )] o Tumor Lysis Syndrome [see Warnings and Precautions ( 5.5 )] Most common adverse reactions (>30%) in adult patients with MDS by subcutaneous route are: nausea, anemia, thrombocytopenia, vomiting, pyrexia, leukopenia, diarrhea, injection site erythema, constipation, neutropenia and ecchymosis. Most common adverse reactions by intravenous route also included petechiae, rigors, weakness and hypokalemia ( 6.1 ). Most common adverse reactions (>30%) by intravenous route in pediatric patients with JMML are pyrexia, rash, upper respiratory tract infection, and anemia ( 6.1 ). To report SUSPECTED ADVERSE REACTIONS, contact Bristol-Myers Squibb at 1-800-721-5072 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch . 6.1 Clinical Trials Experience Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice. MDS The data described below reflect exposure to VIDAZA in 443 patients with MDS from 4 clinical studies. Study 1 was a supportive-care controlled trial (subcutaneous administration), Studies 2 and 3 were single arm studies (one with subcutaneous administration and one with intravenous administration), and Study 4 was an international randomized trial (subcutaneous administration) [see Clinical Studies ( 14.1 )]. In Studies 1, 2 and 3, a total of 268 patients were exposed to VIDAZA, including 116 exposed for 6 cycles (approximately 6 months) or more and 60 exposed for greater than 12 cycles (approximately one year). VIDAZA was studied primarily in supportive-care controlled and uncontrolled trials (n=150 and n=118, respectively). The population in the subcutaneous studies (n=220) was 23 to 92 years old (mean 66.4 years), 68% male, and 94% white, and had MDS or AML. The population in the intravenous study (n=48) was 35 to 81 years old (mean 63.1 years), 65% male, and 100% white. Most patients received average daily doses between 50 and 100 mg/m 2 . In Study 4, a total of 175 patients with higher-risk MDS (primarily RAEB and RAEB-T subtypes) were exposed to VIDAZA. Of these patients, 119 were exposed for 6 or more cycles, and 63 for at least 12 cycles. The mean age of this population was 68.1 years (ranging from 42 to 83 years), 74% were male, and 99% were white. Most patients received daily VIDAZA doses of 75 mg/m 2 . Most Commonly Occurring Adverse Reactions (Subcutaneous or Intravenous Route) in Adult Patients with MDS: nausea, anemia, thrombocytopenia, vomiting, pyrexia, leukopenia, diarrhea, injection site erythema, constipation, neutropenia, ecchymosis. The most common adverse reactions by intravenous route also included petechiae, rigors, weakness and hypokalemia. Adverse Reactions Most Frequently (>2%) Resulting in Clinical Intervention (Subcutaneous or Intravenous Route) in Adult Patients with MDS: Discontinuation: leukopenia, thrombocytopenia, neutropenia. Dose Held: leukopenia, neutropenia, thrombocytopenia, pyrexia, pneumonia, febrile neutropenia. Dose Reduced: leukopenia, neutropenia, thrombocytopenia. Table 3 presents adverse reactions occurring in at least 5% of patients treated with VIDAZA (subcutaneous) in Studies 1 and 2. It is important to note that duration of exposure was longer for the VIDAZA-treated group than for the observation group: patients received VIDAZA for a mean of 11.4 months while mean time in the observation arm was 6.1 months. Table 3: Most Frequently Observed Adverse Reactions (≥ 5% in All Subcutaneous VIDAZA Treated Patients; Studies 1 and 2) Number (%) of Patients System Organ Class Preferred Term a All VIDAZA b (N=220) Observation c (N=92) a Multiple terms of the same preferred terms for a patient are only counted once within each treatment group. b Includes adverse reactions from all patients exposed to VIDAZA, including patients after crossing over from observations. c Includes adverse reactions from observation period only; excludes any adverse events after crossover to VIDAZA. Blood and lymphatic system disorders Anemia 153 (70) 59 (64) Anemia aggravated 12 (6) 5 (5) Febrile neutropenia 36 (16) 4 (4) Leukopenia 106 (48) 27 (29) Neutropenia 71 (32) 10 (11) Thrombocytopenia 144 (66) 42 (46) Gastrointestinal disorders Abdominal tenderness 26 (12) 1 (1) Constipation 74 (34) 6 (7) Diarrhea 80 (36) 13 (14) Gingival bleeding 21 (10) 4 (4) Loose stools 12 (6) 0 Mouth hemorrhage 11 (5) 1 (1) Nausea 155 (71) 16 (17) Stomatitis 17 (8) 0 Vomiting 119 (54) 5 (5) General disorders and administration site conditions Chest pain 36 (16) 5 (5) Injection site bruising 31 (14) 0 Injection site erythema 77 (35) 0 Injection site granuloma 11 (5) 0 Injection site pain 50 (23) 0 Injection site pigmentation changes 11 (5) 0 Injection site pruritus 15 (7) 0 Injection site reaction 30 (14) 0 Injection site swelling 11 (5) 0 Lethargy 17 (8) 2 (2) Malaise 24 (11) 1 (1) Pyrexia 114 (52) 28 (30) Infections and infestations Nasopharyngitis 32 (15) 3 (3) Pneumonia 24 (11) 5 (5) Upper respiratory tract infection 28 (13) 4 (4) Injury, poisoning, and procedural complications Post procedural hemorrhage 13 (6) 1 (1) Metabolism and nutrition disorders Anorexia 45 (21) 6 (7) Musculoskeletal and connective tissue disorders Arthralgia 49 (22) 3 (3) Chest wall pain 11 (5) 0 Myalgia 35 (16) 2 (2) Nervous system disorders Dizziness 41 (19) 5 (5) Headache 48 (22) 10 (11) Psychiatric disorders Anxiety 29 (13) 3 (3) Insomnia 24 (11) 4 (4) Respiratory, thoracic and mediastinal disorders Dyspnea 64 (29) 11 (12) Skin and subcutaneous tissue disorders Dry skin 11 (5) 1 (1) Ecchymosis 67 (31) 14 (15) Erythema 37 (17) 4 (4) Rash 31 (14) 9 (10) Skin nodule 11 (5) 1 (1) Urticaria 13 (6) 1 (1) Vascular disorders Hematoma 19 (9) 0 Hypotension 15 (7) 2 (2) Petechiae 52 (24) 8 (9) Table 4 presents adverse reactions occurring in at least 5% of patients treated with VIDAZA in Study 4. Similar to Studies 1 and 2 described above, duration of exposure to treatment with VIDAZA was longer (mean 12.2 months) compared with best supportive care (mean 7.5 months). Table 4: Most Frequently Observed Adverse Reactions (≥ 5% in the VIDAZA Treated Patients and the Percentage with NCI CTC Grade 3/4 Reactions; Study 4) Number (%) of Patients Any Grade Grade 3/4 System Organ Class Preferred Term a VIDAZA (N=175) Best Supportive Care Only (N=102) VIDAZA (N=175) Best Supportive Care Only (N=102) a Multiple reports of the same preferred term from a patient were only counted once within each treatment. Blood and lymphatic system disorders Anemia 90 (51) 45 (44) 24 (14) 9 (9) Febrile neutropenia 24 (14) 10 (10) 22 (13) 7 (7) Leukopenia 32 (18) 2 (2) 26 (15) 1 (1) Neutropenia 115 (66) 29 (28) 107 (61) 22 (22) Thrombocytopenia 122 (70) 35 (34) 102 (58) 29 (28) Gastrointestinal disorders Abdominal pain 22 (13) 7 (7) 7 (4) 0 Constipation 88 (50) 8 (8) 2 (1) 0 Dyspepsia 10 (6) 2 (2) 0 0 Nausea 84 (48) 12 (12) 3 (2) 0 Vomiting 47 (27) 7 (7) 0 0 General disorders and administration site conditions Fatigue 42 (24) 12 (12) 6 (3) 2 (2) Injection site bruising 9 (5) 0 0 0 Injection site erythema 75 (43) 0 0 0 Injection site hematoma 11 (6) 0 0 0 Injection site induration 9 (5) 0 0 0 Injection site pain 33 (19) 0 0 0 Injection site rash 10 (6) 0 0 0 Injection site reaction 51 (29) 0 1 (1) 0 Pyrexia 53 (30) 18 (18) 8 (5) 1 (1) Infections and infestations Rhinitis 10 (6) 1 (1) 0 0 Upper respiratory tract infection 16 (9) 4 (4) 3 (2) 0 Urinary tract infection 15 (9) 3 (3) 3 (2) 0 Investigations Weight decreased 14 (8) 0 1 (1) 0 Metabolism and nutrition disorders Hypokalemia 11 (6) 3 (3) 3 (2) 3 (3) Nervous system disorders Lethargy 13 (7) 2 (2) 0 1 (1) Psychiatric disorders Anxiety 9 (5) 1 (1) 0 0 Insomnia 15 (9) 3 (3) 0 0 Renal and urinary disorders Hematuria 11 (6) 2 (2) 4 (2) 1 (1) Respiratory, thoracic and mediastinal disorders Dyspnea 26 (15) 5 (5) 6 (3) 2 (2) Dyspnea exertional 9 (5) 1 (1) 0 0 Pharyngolaryngeal pain 11 (6) 3 (3) 0 0 Skin and subcutaneous tissue disorders Erythema 13 (7) 3 (3) 0 0 Petechiae 20 (11) 4 (4) 2 (1) 0 Pruritus 21 (12) 2 (2) 0 0 Rash 18 (10) 1 (1) 0 0 Vascular disorders Hypertension 15 (9) 4 (4) 2 (1) 2 (2) In Studies 1, 2 and 4 with subcutaneous administration of VIDAZA, adverse reactions of neutropenia, thrombocytopenia, anemia, nausea, vomiting, diarrhea, constipation, and injection site erythema/reaction tended to increase in incidence with higher doses of VIDAZA. Adverse reactions that tended to be more pronounced during the first 1 to 2 cycles of subcutaneous treatment compared with later cycles included thrombocytopenia, neutropenia, anemia, nausea, vomiting, injection site erythema/pain/bruising/reaction, constipation, petechiae, dizziness, anxiety, hypokalemia, and insomnia. There did not appear to be any adverse reactions that increased in frequency over the course of treatment. Overall, adverse reactions were qualitatively similar between the intravenous and subcutaneous studies. Adverse reactions that appeared to be specifically associated with the intravenous route of administration included infusion site reactions (e.g. erythema or pain) and catheter site reactions (e.g. infection, erythema, or hemorrhage). In clinical studies of either subcutaneous or intravenous VIDAZA, the following serious adverse reactions occurring at a rate of <5% (and not described in Tables 2 or 3) were reported: Blood and lymphatic system disorders: agranulocytosis, bone marrow failure, pancytopenia splenomegaly. Cardiac disorders: atrial fibrillation, cardiac failure, cardiac failure congestive, cardio-respiratory arrest, congestive cardiomyopathy. Eye disorders: eye hemorrhage Gastrointestinal disorders: diverticulitis, gastrointestinal hemorrhage, melena, perirectal abscess. General disorders and administration site conditions: catheter site hemorrhage, general physical health deterioration, systemic inflammatory response syndrome. Hepatobiliary disorders: cholecystitis. Immune system disorders: anaphylactic shock, hypersensitivity. Infections and infestations: abscess limb, bacterial infection, cellulitis, blastomycosis, injection site infection, Klebsiella sepsis, neutropenic sepsis, pharyngitis streptococcal, pneumonia Klebsiella, sepsis, septic shock, Staphylococcal bacteremia, Staphylococcal infection, toxoplasmosis. Metabolism and nutrition disorders: dehydration. Musculoskeletal and connective tissue disorders: bone pain aggravated, muscle weakness, neck pain. Neoplasms benign, malignant and unspecified: leukemia cutis. Nervous system disorders: cerebral hemorrhage, convulsions, intracranial hemorrhage. Renal and urinary disorders: loin pain, renal failure. Respiratory, thoracic and mediastinal disorders: hemoptysis, lung infiltration, pneumonitis, respiratory distress. Skin and subcutaneous tissue disorders: pyoderma gangrenosum, rash pruritic, skin induration. Surgical and medical procedures: cholecystectomy. Vascular disorders: orthostatic hypotension. Juvenile Myelomonocytic Leukemia (JMML) The safety of VIDAZA was evaluated in pediatric patients with JMML (N=18; 0.2-6.9 years old) in Study AZA-JMML-001 [see Clinical Studies ( 14.2 )] . Patients received VIDAZA as intravenous infusion daily for 7 days in a 28-day cycle [see Dosage and Administration ( 2.4 )] . Sixteen patients completed 3 cycles of therapy and 5 of the 16 patients completed 6 cycles. The median treatment duration was 12.3 weeks (range: 4.0 to 30.6 weeks) and the median total number of treatment cycles completed was 3 cycles (range: 1 to 6 cycles). Serious adverse reactions occurred in 67% of patients who received VIDAZA for JMML. Permanent discontinuation of VIDAZA due to an adverse reaction occurred in a single patient who had abdominal pain and acute respiratory distress syndrome. The most common (≥30%) adverse reactions were pyrexia, rash, upper respiratory tract infection, and anemia. Table 5 summarizes the adverse reactions in pediatric JMML. Table 5: Most Frequently Observed Adverse Reactions (≥10%) in Pediatric Patients with JMML Receiving VIDAZA in Study AZA-JMML-001 Adverse Reaction All Grades N=18 % Grade 3 or 4 N=18 % General disorders and administration site conditions Pyrexia 61 0 Edema a 11 0 Skin and subcutaneous tissue disorders Rash b 44 0 Pruritus c 22 0 Dermatitis allergic 11 0 Petechiae 11 0 Infections and infestations Upper respiratory tract infection d 44 6 Febrile infection 11 6 Fungal infection e 11 6 Pneumonia f 11 0 Blood and lymphatic system disorders Anemia 39 33 Thrombocytopenia 28 22 Neutropenia 17 11 Febrile Neutropenia 11 6 Lymphadenopathy 11 6 Gastrointestinal disorders Vomiting 28 0 Abdominal pain g 22 11 Constipation 22 0 Diarrhea 22 6 Hemorrhage h 11 0 Nausea 11 0 Ascites 11 6 Respiratory, thoracic and mediastinal disorders Cough 22 0 Epistaxis 17 6 Metabolism and nutrition disorders Hyperuricemia 17 0 Fluid retention 11 0 Musculoskeletal and connective tissue disorders Musculoskeletal pain i 11 0 a Grouped term includes: face edema, generalized edema, edema peripheral. b Grouped term includes: rash, rash macular, dermatitis bullous, rash maculo-papular, rash papular, rash pruritic. c Grouped term includes: pruritis, pruritis generalized. d Grouped term includes: influenza, nasopharyngitis, Parainfluenzae virus infection, respiratory tract infection, rhinitis, upper respiratory tract infection, and viral upper respiratory tract infection e Grouped term includes: anal candidiasis, Candida infection, oral candidiasis. f Grouped term includes: lung infection, pneumonia respiratory syncytial viral. g Grouped term includes: abdominal pain, abdominal pain upper. h Grouped term includes: mouth hemorrhage, rectal hemorrhage. i Grouped term includes: back pain, musculoskeletal pain, non-cardiac chest pain, pain in extremity. 6.2 Postmarketing Experience The following adverse reactions have been identified during postmarketing use of VIDAZA. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure. ‑ Interstitial lung disease ‑ Tumor lysis syndrome ‑ Injection site necrosis ‑ Sweet's syndrome (acute febrile neutrophilic dermatosis) ‑ Necrotizing fasciitis (including fatal cases) ‑ Differentiation syndrome ‑ Pericardial effusion ‑ Pericarditis

Contraindications

4 CONTRAINDICATIONS • Advanced Malignant Hepatic Tumors ( 4.1 ). • Hypersensitivity to Azacitidine or Mannitol ( 4.2 ). 4.1 Advanced Malignant Hepatic Tumors VIDAZA is contraindicated in patients with advanced malignant hepatic tumors [see Warnings and Precautions ( 5.3 )] . 4.2 Hypersensitivity to Azacitidine or Mannitol VIDAZA is contraindicated in patients with a known hypersensitivity to azacitidine or mannitol.

Description

11 DESCRIPTION VIDAZA (azacitidine for injection) contains azacitidine, which is a nucleoside metabolic inhibitor. Azacitidine is 4-amino-1-β-D-ribofuranosyl-s-triazin-2(1H)-one. The structural formula is as follows: The empirical formula is C 8 H 12 N 4 O 5. The molecular weight is 244. Azacitidine is a white to off-white solid. Azacitidine was found to be insoluble in acetone, ethanol, and methyl ethyl ketone; slightly soluble in ethanol/water (50/50), propylene glycol, and polyethylene glycol; sparingly soluble in water, water saturated octanol, 5% dextrose in water, N-methyl-2-pyrrolidone, normal saline and 5% Tween 80 in water; and soluble in dimethylsulfoxide (DMSO). The finished product is supplied in a sterile form for reconstitution as a suspension for subcutaneous injection or reconstitution as a solution with further dilution for intravenous infusion. Vials of VIDAZA contain 100 mg of azacitidine and 100 mg mannitol as a sterile lyophilized powder. AzacitidineStructuralFormula

Dosage And Administration

2 DOSAGE AND ADMINISTRATION • Do not substitute VIDAZA for oral azacitidine. The indications and dosing regimen for VIDAZA differ from that of oral azacitidine ( 2.1 , 5.1 ). • MDS: The recommended starting dosage for the first treatment cycle, for all patients regardless of baseline hematology values, is VIDAZA 75 mg/m 2 daily for 7 days to be administered by subcutaneous injection or intravenous infusion. See full prescribing information for schedule for subsequent cycles. Premedicate for nausea and vomiting ( 2.2 ). • JMML: See full prescribing information for recommended dosage and schedule. • Continue treatment as long as the patient continues to benefit; up to 6 cycles for pediatric patients with JMML ( 2.3 , 2.4 ). • Monitor all patients for hematologic response and for renal toxicity; delay or reduce dosage as appropriate ( 2.3 , 2.4 , 2.6 , 2.7 ). 2.1 Important Administration Information Do not substitute VIDAZA for oral azacitidine. The indications and dosing regimen for VIDAZA differ from that of oral azacitidine [see Warnings and Precautions ( 5.1 )] 2.2 First Treatment Cycle for Adults The recommended starting dose for the first treatment cycle, for all patients regardless of baseline hematology laboratory values, is 75 mg/m 2 subcutaneously or intravenously, daily for 7 days. Premedicate patients for nausea and vomiting. Obtain complete blood counts, liver chemistries and serum creatinine prior to the first dose. 2.3 Subsequent Treatment Cycles for Adults Repeat cycles every 4 weeks. The dose may be increased to 100 mg/m 2 if no beneficial effect is seen after 2 treatment cycles and if no toxicity other than nausea and vomiting has occurred. It is recommended that patients be treated for a minimum of 4 to 6 cycles. However, complete or partial response may require additional treatment cycles. Treatment may be continued as long as the patient continues to benefit. Monitor patients for hematologic response and renal toxicities [see Warnings and Precautions ( 5.4 )], and delay or reduce dosage if necessary [see Dosage and Administration ( 2.6 )]. 2.4 Pediatric Patients with JMML Table 1: Dosage and Administration for Pediatric Patients (JMML) Pediatric Patients with JMML Recommended Dose Age 1 month to less than 1 year OR weighing less than 10 kg 2.5 mg/kg Age 1 year and older AND weighing 10 kg or greater 75 mg/m2 The recommended dosage for pediatric patients with JMML is provided in Table 1. VIDAZA is administered as an intravenous infusion daily for 7 days in a 28-day cycle. Patients should be treated for a minimum of 3 cycles and maximum of 6 cycles. A delay in dose not exceeding 14 days can be considered for non-hematologic toxicities. Monitor patients for hematologic response and renal toxicities [see Warnings and Precautions ( 5.4 )], and delay or reduce dosage if necessary. Treatment may be continued up to six cycles as long as the patient continues to benefit. 2.5 Dosage Adjustment Based on Hematology Laboratory Values • For adult patients with baseline (start of treatment) WBC greater than or equal to 3 x10 9 /L, ANC greater than or equal to 1.5 x10 9 /L, and platelets greater than or equal to 75 x10 9 /L, adjust the dose as follows, based on nadir counts for any given cycle: Nadir Counts % Dose in the Next Course ANC (x10 9 /L) Less than 0.5 0.5 –1.5 Greater than 1.5 Platelets (x10 9 /L) Less than 25 25-50 Greater than 50 50% 67% 100% • For adult patients whose baseline counts are WBC less than 3 x10 9 /L, ANC less than 1.5 x10 9 /L, or platelets less than 75 x10 9 /L, base dose adjustments on nadir counts and bone marrow biopsy cellularity at the time of the nadir as noted below, unless there is clear improvement in differentiation (percentage of mature granulocytes is higher and ANC is higher than at onset of that course) at the time of the next cycle, in which case continue the current dose. WBC or Platelet Nadir % decrease in counts from baseline Bone Marrow Biopsy Cellularity at Time of Nadir (%) 30-60 15-30 Less than 15 % Dose in the Next Course 50 - 75 100 50 33 Greater than 75 75 50 33 If a nadir as defined in the table above has occurred, give the next course 28 days after the start of the preceding course, provided that both the WBC and the platelet counts are greater than 25% above the nadir and rising. If a greater than 25% increase above the nadir is not seen by day 28, reassess counts every 7 days. If a 25% increase is not seen by day 42, reduce the scheduled dose by 50%. Pediatric Patients with JMML As hematological toxicity will be difficult to assess and to differentiate from the natural course of the underlying disorder, dose reductions are not recommended due to hematological toxicity within the first 3 cycles. However, if the patient has a neutrophil count of less than 0.5 x109/L at end of Cycle 3 or on Day 1 of Cycles 5 or 6, discontinue the treatment. 2.6 Dosage Adjustment Based on Serum Electrolytes and Renal Toxicity If unexplained reductions in serum bicarbonate levels to less than 20 mEq/L occur, reduce the dosage by 50% for the next course. Similarly, if unexplained elevations of BUN or serum creatinine occur, delay the next cycle until values return to normal or baseline and reduce the dose by 50% for the next course [see Warnings and Precautions ( 5.4 )]. 2.7 Use in Geriatric Patients Azacitidine and its metabolites are known to be substantially excreted by the kidney, and the risk of toxic reactions to this drug may be greater in patients with impaired renal function. Because elderly patients are more likely to have decreased renal function, select the dose carefully and monitor renal function [see Warnings and Precautions ( 5.4 ) and Use in Specific Populations ( 8.5 )]. 2.8 Preparation of VIDAZA VIDAZA is a hazardous drug. Follow applicable special handling and disposal procedures. 1 The VIDAZA vial is single-dose and does not contain any preservatives. Discard unused portions of each vial properly [see How Supplied/Storage and Handling ( 16 )]. Do not save any unused portions for later administration. 2.9 Instructions for Subcutaneous Administration Reconstitute VIDAZA aseptically with 4 mL Sterile Water for Injection, USP to obtain a concentration of 25 mg/mL. Inject the diluent slowly into the vial. Vigorously shake or roll the vial until a uniform suspension is achieved. The suspension will be cloudy. Do not filter the suspension after reconstitution. Doing so could remove the active substance. Preparation for Immediate Subcutaneous Administration: For doses requiring more than 1 vial, divide the dose equally between the syringes (e.g., dose 150 mg = 6 mL, 2 syringes with 3 mL in each syringe) and inject into two separate sites. Due to retention in the vial and needle, it may not be feasible to withdraw all of the suspension from the vial. The product may be held at room temperature for up to 1 hour, but must be administered within 1 hour after reconstitution. Preparation for Delayed Subcutaneous Administration: The reconstituted product may be kept in the vial or drawn into a syringe. For doses requiring more than 1 vial, divide the dose equally between the syringes (e.g., dose 150 mg = 6 mL, 2 syringes with 3 mL in each syringe) and inject into two separate sites. Due to retention in the vial and needle, it may not be feasible to withdraw all of the suspension from the vial. The product must be refrigerated immediately. See Table 2 for suspension stability storage timelines based on the temperature of the diluent for delayed subcutaneous administration. After removal from refrigerated conditions, the suspension may be allowed to equilibrate to room temperature for up to 30 minutes prior to administration. Subcutaneous Administration To provide a homogeneous suspension, the contents of the dosing syringe must be re-suspended immediately prior to administration. To re-suspend, vigorously roll the syringe between the palms until a uniform, cloudy suspension is achieved. VIDAZA suspension is administered subcutaneously. Rotate sites for each injection (thigh, abdomen, or upper arm). New injections should be given at least one inch from an old site and never into areas where the site is tender, bruised, red, or hard. Table 2 Suspension Stability: Storage timelines based on the temperature of the diluent for suspension stability storage: Suspension Stability Storage timelines Diluent Storage Temperature/Duration Room temperature (25°C / 77°F) Sterile Water for Injection, USP Store at room temperature at 25°C (77°F) for up to 1 hour or refrigerated at 2°C to 8°C (36°F to 46°F) for up to 8 hours. Cold (2°C to 8°C / 36°F to 46°F) Sterile Water for Injection, USP Store refrigerated at 2°C to 8°C (36°F to 46°F) for up to 22 hours. 2.10 Instructions for Intravenous Administration Parenteral drug product should be inspected visually for particulate matter and discoloration prior to administration, whenever solution and container permit. Do not use the product if there is evidence of particulate matter or discoloration. Adult Patients with MDS Reconstitute the appropriate number of VIDAZA vials to achieve the desired dose. Reconstitute each vial with 10 mL Sterile Water for Injection, USP. Vigorously shake or roll the vial until all solids are dissolved. The resulting solution will contain azacitidine 10 mg/mL. The solution should be clear. Withdraw the required amount of VIDAZA solution to deliver the desired dose and inject into a 50 -100 mL infusion bag of either 0.9% Sodium Chloride Injection, USP or Lactated Ringer’s Injection, USP. Pediatric Patients with JMML For pediatric patients with JMML, withdraw the required amount of VIDAZA solution to deliver the desired dose and inject into an infusion bag (volume up to 100 mL) of either 0.9% Sodium Chloride Injection, USP or Lactated Ringer’s Injection, USP to achieve a final VIDAZA concentration between 0.9 mg/mL and 4 mg/mL. Intravenous Solution Incompatibility VIDAZA is incompatible with 5% Dextrose Injection, USP solutions, Hespan, or solutions that contain bicarbonate. These solutions have the potential to increase the rate of degradation of VIDAZA and should therefore be avoided. Intravenous Administration VIDAZA solution is administered intravenously. Administer the total dose over a period of 10 - 40 minutes. The administration must be completed within 1 hour of reconstitution of the VIDAZA vial. Solution Stability : VIDAZA reconstituted and diluted for intravenous administration may be stored at 25°C (77°F), but administration must be completed within 1 hour of reconstitution.

Indications And Usage

1 INDICATIONS AND USAGE VIDAZA is a nucleoside metabolic inhibitor indicated for the treatment of: • Adult patients with the following FAB myelodysplastic syndrome (MDS) subtypes: Refractory anemia (RA) or refractory anemia with ringed sideroblasts (RARS) (if accompanied by neutropenia or thrombocytopenia or requiring transfusions), refractory anemia with excess blasts (RAEB), refractory anemia with excess blasts in transformation (RAEB-T), and chronic myelomonocytic leukemia (CMMoL). ( 1.1 ) • Pediatric patients aged 1 month and older with newly diagnosed Juvenile Myelomonocytic Leukemia (JMML). ( 1.2 ) 1.1 Myelodysplastic Syndromes (MDS) VIDAZA ® is indicated for treatment of adult patients with the following French-American-British (FAB) myelodysplastic syndrome subtypes: refractory anemia (RA) or refractory anemia with ringed sideroblasts (if accompanied by neutropenia or thrombocytopenia or requiring transfusions), refractory anemia with excess blasts (RAEB), refractory anemia with excess blasts in transformation (RAEB-T), and chronic myelomonocytic leukemia (CMMoL). 1.2 Juvenile Myelomonocytic Leukemia (JMML) VIDAZA is indicated for the treatment of pediatric patients aged one month and older with newly diagnosed JMML.

Overdosage

10 OVERDOSAGE One case of overdose with VIDAZA was reported during clinical trials. A patient experienced diarrhea, nausea, and vomiting after receiving a single intravenous dose of approximately 290 mg/m 2 , almost 4 times the recommended starting dose. The events resolved without sequelae, and the correct dose was resumed the following day. In the event of overdosage, the patient should be monitored with appropriate blood counts and should receive supportive treatment, as necessary. There is no known specific antidote for VIDAZA overdosage.

Adverse Reactions Table

Table 3: Most Frequently Observed Adverse Reactions (≥ 5% in All Subcutaneous VIDAZA Treated Patients; Studies 1 and 2)
Number (%) of Patients
System Organ Class Preferred TermaAll VIDAZAb (N=220)Observationc (N=92)
a Multiple terms of the same preferred terms for a patient are only counted once within each treatment group. b Includes adverse reactions from all patients exposed to VIDAZA, including patients after crossing over from observations. c Includes adverse reactions from observation period only; excludes any adverse events after crossover to VIDAZA.

Blood and lymphatic system disorders

Anemia

153 (70)

59 (64)

Anemia aggravated

12 (6)

5 (5)

Febrile neutropenia

36 (16)

4 (4)

Leukopenia

106 (48)

27 (29)

Neutropenia

71 (32)

10 (11)

Thrombocytopenia

144 (66)

42 (46)

Gastrointestinal disorders

Abdominal tenderness

26 (12)

1 (1)

Constipation

74 (34)

6 (7)

Diarrhea

80 (36)

13 (14)

Gingival bleeding

21 (10)

4 (4)

Loose stools

12 (6)

0

Mouth hemorrhage

11 (5)

1 (1)

Nausea

155 (71)

16 (17)

Stomatitis

17 (8)

0

Vomiting

119 (54)

5 (5)

General disorders and administration site conditions

Chest pain

36 (16)

5 (5)

Injection site bruising

31 (14)

0

Injection site erythema

77 (35)

0

Injection site granuloma

11 (5)

0

Injection site pain

50 (23)

0

Injection site pigmentation changes

11 (5)

0

Injection site pruritus

15 (7)

0

Injection site reaction

30 (14)

0

Injection site swelling

11 (5)

0

Lethargy

17 (8)

2 (2)

Malaise

24 (11)

1 (1)

Pyrexia

114 (52)

28 (30)

Infections and infestations

Nasopharyngitis

32 (15)

3 (3)

Pneumonia

24 (11)

5 (5)

Upper respiratory tract infection

28 (13)

4 (4)

Injury, poisoning, and procedural complications

Post procedural hemorrhage

13 (6)

1 (1)

Metabolism and nutrition disorders

Anorexia

45 (21)

6 (7)

Musculoskeletal and connective tissue disorders

Arthralgia

49 (22)

3 (3)

Chest wall pain

11 (5)

0

Myalgia

35 (16)

2 (2)

Nervous system disorders

Dizziness

41 (19)

5 (5)

Headache

48 (22)

10 (11)

Psychiatric disorders

Anxiety

29 (13)

3 (3)

Insomnia

24 (11)

4 (4)

Respiratory, thoracic and mediastinal disorders

Dyspnea

64 (29)

11 (12)

Skin and subcutaneous tissue disorders

Dry skin

11 (5)

1 (1)

Ecchymosis

67 (31)

14 (15)

Erythema

37 (17)

4 (4)

Rash

31 (14)

9 (10)

Skin nodule

11 (5)

1 (1)

Urticaria

13 (6)

1 (1)

Vascular disorders

Hematoma

19 (9)

0

Hypotension

15 (7)

2 (2)

Petechiae

52 (24)

8 (9)

Clinical Pharmacology

12 CLINICAL PHARMACOLOGY 12.1 Mechanism of Action VIDAZA is a pyrimidine nucleoside analog of cytidine. VIDAZA is believed to exert its antineoplastic effects by causing hypomethylation of DNA and direct cytotoxicity on abnormal hematopoietic cells in the bone marrow. The concentration of azacitidine required for maximum inhibition of DNA methylation in vitro does not cause major suppression of DNA synthesis. Hypomethylation may restore normal function to genes that are critical for differentiation and proliferation. The cytotoxic effects of azacitidine cause the death of rapidly dividing cells, including cancer cells that are no longer responsive to normal growth control mechanisms. Non-proliferating cells are relatively insensitive to azacitidine. 12.2 Pharmacodynamics In pediatric patients with JMML post azacitidine treatment (75 mg/m 2 or 2.5 mg/kg), reductions in genome-wide DNA methylation (global DNA methylation scores) were attained in bone marrow granulocytes during the first treatment cycle, confirming the DNA-hypomethylating activity of azacitidine. 12.3 Pharmacokinetics The pharmacokinetics of azacitidine were studied in 6 adult patients with MDS following a single 75 mg/m 2 subcutaneous dose and a single 75 mg/m 2 intravenous dose. Absorption Azacitidine is rapidly absorbed after subcutaneous administration; the peak plasma azacitidine concentration of 750 ± 403 ng/ml occurred in 0.5 hour after subcutaneous administration. Distribution The bioavailability of subcutaneous azacitidine relative to intravenous azacitidine is approximately 89%, based on area under the curve. Mean volume of distribution following intravenous dosing is 76 ± 26 L. Mean apparent subcutaneous clearance is 167 ± 49 L/hour and mean half-life after subcutaneous administration is 41 ± 8 minutes. The AUC and C max of subcutaneous administration of azacitidine in 21 patients with cancer were approximately dose proportional within the 25 to 100 mg/m 2 dose range. Multiple dosing at the recommended dose-regimen does not result in drug accumulation with intravenous or subcutaneous administration. Elimination Metabolism An in vitro study of azacitidine incubation in human liver fractions indicated that azacitidine is not metabolized by the cytochrome P450 (CYP) enzymes. Azacitidine undergoes spontaneous hydrolysis and deamination mediated by cytidine deaminase. Excretion Published studies indicate that urinary excretion is the primary route of elimination of azacitidine and its metabolites. Following intravenous administration of radioactive azacitidine to 5 cancer patients, the cumulative urinary excretion was 85% of the radioactive dose. Fecal excretion accounted for <1% of administered radioactivity over 3 days. Mean excretion of radioactivity in urine following subcutaneous administration of 14 C-azacitidine was 50%. The mean elimination half-lives of total radioactivity (azacitidine and its metabolites) were similar after intravenous and subcutaneous administrations, about 4 hours. Specific Populations The effects of hepatic impairment, gender, or race/ethnicity on the pharmacokinetics of intravenous and subcutaneous azacitidine have not been studied. Pediatric Patients Following intravenous administration of a 75 mg/m 2 or 2.5 mg/kg dose in pediatric patients with JMML, population pharmacokinetic analysis determined that azacitidine rapidly reached a geometric mean C max of 4510 ng/mL (CV%: 65.6%), and a geometric mean AUC 0-24 of 1550 ng∙h/mL (CV%: 56.6%). The geometric mean t 1/2 was 0.3 hours (CV%: 59.9%), and the geometric mean clearance was 21.8 L/h (CV%: 102.2%). Population PK analysis of 6 adults and 34 pediatric patients did not identify any clinically meaningful differences in the pharmacokinetics of intravenous azacitidine according to sex (62.5% male), and tumor type (MDS, JMML, AML). Increased clearance was associated with increased baseline body weight (4.6 to 102 kg). BSA or body weight-based dosing resulted in consistent plasma azacitidine exposure in pediatric patients with JMML across the body weight range (4.6 to 18.5 kg) and age range (0.2 to 6.9 years). Patients with Renal Impairment In adult patients with cancer, the pharmacokinetics of azacitidine in 6 patients with normal renal function (CLcr >80 mL/min) and 6 patients with severe renal impairment (CLcr <30 mL/min) were compared following daily subcutaneous dosing (Days 1 through 5) at 75 mg/m 2 /day. Severe renal impairment increased azacitidine exposure by approximately 70% after single and 41% after multiple subcutaneous administrations. This increase in exposure was not correlated with an increase in adverse events. The exposure was similar to exposure in patients with normal renal function receiving 100 mg/m 2 . Drug-Drug Interactions No formal clinical drug interaction studies with azacitidine have been conducted. In vitro Studies Cytochrome P450 (CYP) Enzymes: An in vitro study at azacitidine concentrations up to 100 µM (IV Cmax = 10.6 µM) in human liver microsomes indicated that azacitidine does not cause any inhibition of CYP isoforms CYP1A2, CYP2B6, CYP2C8, CYP2C9, CYP2C19, CYP2D6, CYP3A4, or CYP2E1 at clinically achievable concentrations. In vitro studies with human cultured hepatocytes indicate that azacitidine at concentrations of 1.0 μM to 100 μM does not induce CYP 1A2, 2C19, or 3A4/5. Transporter Systems: An in vitro study with LLC-PK1 cells expressing P-glycoprotein (P-gp) indicated that azacitidine is not a substrate or inhibitor of P-gp. Azacitidine does not inhibit, breast cancer resistance protein (BCRP), organic anion transporters (OAT) OAT1 and OAT3, organic anion transporting polypeptides (OATP) OATP1B1 and OATP1B3, or organic cation transporter (OCT) OCT2 at clinically relevant concentrations.

Mechanism Of Action

12.1 Mechanism of Action VIDAZA is a pyrimidine nucleoside analog of cytidine. VIDAZA is believed to exert its antineoplastic effects by causing hypomethylation of DNA and direct cytotoxicity on abnormal hematopoietic cells in the bone marrow. The concentration of azacitidine required for maximum inhibition of DNA methylation in vitro does not cause major suppression of DNA synthesis. Hypomethylation may restore normal function to genes that are critical for differentiation and proliferation. The cytotoxic effects of azacitidine cause the death of rapidly dividing cells, including cancer cells that are no longer responsive to normal growth control mechanisms. Non-proliferating cells are relatively insensitive to azacitidine.

Pharmacodynamics

12.2 Pharmacodynamics In pediatric patients with JMML post azacitidine treatment (75 mg/m 2 or 2.5 mg/kg), reductions in genome-wide DNA methylation (global DNA methylation scores) were attained in bone marrow granulocytes during the first treatment cycle, confirming the DNA-hypomethylating activity of azacitidine.

Pharmacokinetics

12.3 Pharmacokinetics The pharmacokinetics of azacitidine were studied in 6 adult patients with MDS following a single 75 mg/m 2 subcutaneous dose and a single 75 mg/m 2 intravenous dose. Absorption Azacitidine is rapidly absorbed after subcutaneous administration; the peak plasma azacitidine concentration of 750 ± 403 ng/ml occurred in 0.5 hour after subcutaneous administration. Distribution The bioavailability of subcutaneous azacitidine relative to intravenous azacitidine is approximately 89%, based on area under the curve. Mean volume of distribution following intravenous dosing is 76 ± 26 L. Mean apparent subcutaneous clearance is 167 ± 49 L/hour and mean half-life after subcutaneous administration is 41 ± 8 minutes. The AUC and C max of subcutaneous administration of azacitidine in 21 patients with cancer were approximately dose proportional within the 25 to 100 mg/m 2 dose range. Multiple dosing at the recommended dose-regimen does not result in drug accumulation with intravenous or subcutaneous administration. Elimination Metabolism An in vitro study of azacitidine incubation in human liver fractions indicated that azacitidine is not metabolized by the cytochrome P450 (CYP) enzymes. Azacitidine undergoes spontaneous hydrolysis and deamination mediated by cytidine deaminase. Excretion Published studies indicate that urinary excretion is the primary route of elimination of azacitidine and its metabolites. Following intravenous administration of radioactive azacitidine to 5 cancer patients, the cumulative urinary excretion was 85% of the radioactive dose. Fecal excretion accounted for <1% of administered radioactivity over 3 days. Mean excretion of radioactivity in urine following subcutaneous administration of 14 C-azacitidine was 50%. The mean elimination half-lives of total radioactivity (azacitidine and its metabolites) were similar after intravenous and subcutaneous administrations, about 4 hours. Specific Populations The effects of hepatic impairment, gender, or race/ethnicity on the pharmacokinetics of intravenous and subcutaneous azacitidine have not been studied. Pediatric Patients Following intravenous administration of a 75 mg/m 2 or 2.5 mg/kg dose in pediatric patients with JMML, population pharmacokinetic analysis determined that azacitidine rapidly reached a geometric mean C max of 4510 ng/mL (CV%: 65.6%), and a geometric mean AUC 0-24 of 1550 ng∙h/mL (CV%: 56.6%). The geometric mean t 1/2 was 0.3 hours (CV%: 59.9%), and the geometric mean clearance was 21.8 L/h (CV%: 102.2%). Population PK analysis of 6 adults and 34 pediatric patients did not identify any clinically meaningful differences in the pharmacokinetics of intravenous azacitidine according to sex (62.5% male), and tumor type (MDS, JMML, AML). Increased clearance was associated with increased baseline body weight (4.6 to 102 kg). BSA or body weight-based dosing resulted in consistent plasma azacitidine exposure in pediatric patients with JMML across the body weight range (4.6 to 18.5 kg) and age range (0.2 to 6.9 years). Patients with Renal Impairment In adult patients with cancer, the pharmacokinetics of azacitidine in 6 patients with normal renal function (CLcr >80 mL/min) and 6 patients with severe renal impairment (CLcr <30 mL/min) were compared following daily subcutaneous dosing (Days 1 through 5) at 75 mg/m 2 /day. Severe renal impairment increased azacitidine exposure by approximately 70% after single and 41% after multiple subcutaneous administrations. This increase in exposure was not correlated with an increase in adverse events. The exposure was similar to exposure in patients with normal renal function receiving 100 mg/m 2 . Drug-Drug Interactions No formal clinical drug interaction studies with azacitidine have been conducted. In vitro Studies Cytochrome P450 (CYP) Enzymes: An in vitro study at azacitidine concentrations up to 100 µM (IV Cmax = 10.6 µM) in human liver microsomes indicated that azacitidine does not cause any inhibition of CYP isoforms CYP1A2, CYP2B6, CYP2C8, CYP2C9, CYP2C19, CYP2D6, CYP3A4, or CYP2E1 at clinically achievable concentrations. In vitro studies with human cultured hepatocytes indicate that azacitidine at concentrations of 1.0 μM to 100 μM does not induce CYP 1A2, 2C19, or 3A4/5. Transporter Systems: An in vitro study with LLC-PK1 cells expressing P-glycoprotein (P-gp) indicated that azacitidine is not a substrate or inhibitor of P-gp. Azacitidine does not inhibit, breast cancer resistance protein (BCRP), organic anion transporters (OAT) OAT1 and OAT3, organic anion transporting polypeptides (OATP) OATP1B1 and OATP1B3, or organic cation transporter (OCT) OCT2 at clinically relevant concentrations.

Effective Time

20220923

Version

21

Dosage And Administration Table

Pediatric Patients with JMML

Recommended Dose

Age 1 month to less than 1 year OR

weighing less than 10 kg

2.5 mg/kg

Age 1 year and older AND weighing 10 kg

or greater

75 mg/m2

Dosage Forms And Strengths

3 DOSAGE FORMS AND STRENGTHS VIDAZA (azacitidine for injection) is supplied as lyophilized powder in 100 mg single-dose vials. • Lyophilized powder in 100 mg single-dose vials ( 3 ).

Spl Product Data Elements

VIDAZA azacitidine AZACITIDINE AZACITIDINE

Nonclinical Toxicology

13 NONCLINICAL TOXICOLOGY 13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility The potential carcinogenicity of azacitidine was evaluated in mice and rats. Azacitidine induced tumors of the hematopoietic system in female mice at 2.2 mg/kg (6.6 mg/m 2 , approximately 8% the recommended human daily dose on a mg/m 2 basis) administered IP three times per week for 52 weeks. An increased incidence of tumors in the lymphoreticular system, lung, mammary gland, and skin was seen in mice treated with azacitidine IP at 2.0 mg/kg (6.0 mg/m 2 , approximately 8% the recommended human daily dose on a mg/m 2 basis) once a week for 50 weeks. A tumorigenicity study in rats dosed twice weekly at 15 or 60 mg/m 2 (approximately 20%-80% the recommended human daily dose on a mg/m 2 basis) revealed an increased incidence of testicular tumors compared with controls. The mutagenic and clastogenic potential of azacitidine was tested in in vitro bacterial systems Salmonella typhimurium strains TA100 and several strains of trpE8, Escherichia coli strains WP14 Pro, WP3103P, WP3104P, and CC103; in in vitro forward gene mutation assay in mouse lymphoma cells and human lymphoblast cells; and in an in vitro micronucleus assay in mouse L5178Y lymphoma cells and Syrian hamster embryo cells. Azacitidine was mutagenic in bacterial and mammalian cell systems. The clastogenic effect of azacitidine was shown by the induction of micronuclei in L5178Y mouse cells and Syrian hamster embryo cells. Administration of azacitidine to male mice at 9.9 mg/m 2 (approximately 9% the recommended human daily dose on a mg/m 2 basis) daily for 3 days prior to mating with untreated female mice resulted in decreased fertility and loss of offspring during subsequent embryonic and postnatal development. Treatment of male rats 3 times per week for 11 or 16 weeks at doses of 15-30 mg/m 2 (approximately 20%-40%, the recommended human daily dose on a mg/m 2 basis) resulted in decreased weight of the testes and epididymides, and decreased sperm counts accompanied by decreased pregnancy rates and increased loss of embryos in mated females. In a related study, male rats treated for 16 weeks at 24 mg/m 2 resulted in an increase in abnormal embryos in mated females when examined on day 2 of gestation.

Application Number

NDA050794

Brand Name

VIDAZA

Generic Name

azacitidine

Product Ndc

59572-102

Product Type

HUMAN PRESCRIPTION DRUG

Route

INTRAVENOUS,SUBCUTANEOUS

Package Label Principal Display Panel

Package Label - Principal Display Panel - 100 mg Vial Label vidaza-label

Recent Major Changes

Indications and Usage, JMML ( 1.2 ) 5/2022 Dosage and Administration ( 2.1 , 2.4 , 2.5 , 2.10 ) 5/2022 Warnings and Precautions ( 5.1 , 5.2 , 5.3 , 5.4 , 5.6 ) 5/2022

Information For Patients

17 PATIENT COUNSELING INFORMATION Hepatotoxicity in Patients with Severe Pre-Existing Hepatic Impairment Instruct patients to inform their physician about any underlying liver disease [see Warnings and Precautions ( 5.3 )]. Renal Toxicity Instruct patients to inform their physician about any underlying renal disease [see Warnings and Precautions ( 5.4 )]. Embryo-Fetal Toxicity Advise pregnant women of the potential risk to a fetus [see Warnings and Precautions ( 5.6 ) and Use in Specific Populations ( 8.1 )]. Advise females of reproductive potential to use effective contraception during treatment with VIDAZA and for 6 months after the last dose. Advise males with female partners of reproductive potential to use effective contraception during treatment with VIDAZA and for 3 months after the last dose. Advise patients to report known or suspected pregnancy to their physicians immediately [see Warnings and Precautions ( 5.6 ) and Use in Specific Populations ( 8.3 )]. Lactation Advise patients to avoid breastfeeding while receiving VIDAZA and for 1 week after the last dose [see Use in Specific Populations ( 8.2 )]. Infertility Advise males and females that VIDAZA may impair fertility [see Use in Specific Populations ( 8.3 ) and Nonclinical Toxicology ( 13.1 )] . Marketed by: Bristol-Myers Squibb Company Princeton, NJ 08543 USA VIDAZA ® is a trademark of Celgene Corporation, a Bristol-Myers Squibb company. VIDPI.18

Information For Patients Table

Marketed by:

Bristol-Myers Squibb Company

Princeton, NJ 08543 USA

Clinical Studies

14 CLINICAL STUDIES 14.1 Myelodysplastic Syndromes (MDS) Study 1 was a randomized, open-label, controlled trial carried out in 53 U.S. sites compared the safety and efficacy of subcutaneous VIDAZA plus supportive care with supportive care alone (“observation”) in adult patients with any of the five FAB subtypes of myelodysplastic syndromes (MDS): refractory anemia (RA), RA with ringed sideroblasts (RARS), RA with excess blasts (RAEB), RAEB in transformation (RAEB-T), and chronic myelomonocytic leukemia (CMMoL). RA and RARS patients were included if they met one or more of the following criteria: required packed RBC transfusions; had platelet counts ≤50.0 x 10 9 /L; required platelet transfusions; or were neutropenic (ANC <1.0 x 10 9 /L) with infections requiring treatment with antibiotics. Patients with acute myelogenous leukemia (AML) were not intended to be included. Supportive care allowed in this study included blood transfusion products, antibiotics, antiemetics, analgesics and antipyretics. The use of hematopoietic growth factors was prohibited. Baseline patient and disease characteristics are summarized in Table 6; the 2 groups were similar. VIDAZA was administered at a subcutaneous dose of 75 mg/m 2 daily for 7 days every 4 weeks. The dose was increased to 100 mg/m 2 if no beneficial effect was seen after 2 treatment cycles. The dose was decreased and/or delayed based on hematologic response or evidence of renal toxicity. Patients in the observation arm were allowed by protocol to cross over to VIDAZA if they had increases in bone marrow blasts, decreases in hemoglobin, increases in red cell transfusion requirements, or decreases in platelets, or if they required a platelet transfusion or developed a clinical infection requiring treatment with antibiotics. For purposes of assessing efficacy, the primary endpoint was response rate (as defined in Table 7). Of the 191 patients included in the study, independent review (adjudicated diagnosis) found that 19 had the diagnosis of AML at baseline. These patients were excluded from the primary analysis of response rate, although they were included in an intent-to-treat (ITT) analysis of all patients randomized. Approximately 55% of the patients randomized to observation crossed over to receive VIDAZA treatment. Table 6 Baseline Demographics and Disease Characteristics VIDAZA (N=99) Observation (N=92) Gender (n%) Male 72 (72.7) 60 (65.2) Female 27 (27.3) 32 (34.8) Race (n%) White 93 (93.9) 85 (92.4) Black 1 (1.0) 1 (1.1) Hispanic 3 (3.0) 5 (5.4) Asian/Oriental 2 (2.0) 1 (1.1) Age (years) N 99 91 Mean ± SD 67.3 ± 10.39 68.0 ± 10.23 Range 31 - 92 35 - 88 Adjudicated MDS diagnosis at study entry (n%) RA 21 (21.2) 18 (19.6) RARS 6 (6.1) 5 (5.4) RAEB 38 (38.4) 39 (42.4) RAEB-T 16 (16.2) 14 (15.2) CMMoL 8 (8.1) 7 (7.6) AML 10 (10.1) 9 (9.8) Transfusion product used in 3 months before study entry (n%) Any transfusion product 70 (70.7) 59 (64.1) Blood cells, packed human 66 (66.7) 55 (59.8) Platelets, human blood 15 (15.2) 12 (13.0) Hetastarch 0(0.0) 1(1.1) Plasma protein fraction 1(1.0) 0(0.0) Other 2(2.0) 2(2.2) Table 7. Response Criteria RA RARS RAEB RAEB-T CMMoL Complete Response (CR), duration ≥4 weeks Marrow <5% blasts Peripheral Blood Normal CBC if abnormal at baseline Absence of blasts in the peripheral circulation Partial Response (PR), duration ≥4 weeks Marrow No marrow requirements ≥50% decrease in blasts Improvement of marrow dyspoiesis Peripheral Blood ≥50% restoration in the deficit from normal levels of baseline white cells, hemoglobin and platelets if abnormal at baseline No blasts in the peripheral circulation For CMMoL, if WBC is elevated at baseline, a ≥75% reduction in the excess count over the upper limit of normal The overall response rate (CR + PR) of 15.7% in VIDAZA-treated patients without AML (16.2% for all VIDAZA randomized patients including AML) was statistically significantly higher than the response rate of 0% in the observation group (p<0.0001) (Table 8). The majority of patients who achieved either CR or PR had either 2 or 3 cell line abnormalities at baseline (79%; 11/14) and had elevated bone marrow blasts or were transfusion dependent at baseline. Patients responding to VIDAZA had a decrease in bone marrow blasts percentage, or an increase in platelets, hemoglobin or WBC. Greater than 90% of the responders initially demonstrated these changes by the 5 th treatment cycle. All patients who had been transfusion dependent became transfusion independent during PR or CR. The mean and median duration of clinical response of PR or better was estimated as 512 and 330 days, respectively; 75% of the responding patients were still in PR or better at completion of treatment. Response occurred in all MDS subtypes as well as in patients with adjudicated baseline diagnosis of AML. Table 8. Response Rates VIDAZA (N=89) Observation Before Crossover (N=83) Response n (%) n (%) P value Overall (CR+PR) 14 (15.7) 0 ( 0.0) (<0.0001) Complete (CR) 5 ( 5.6) 0 ( 0.0) (0.06) Partial (PR) 9 (10.1) 0 ( 0.0) -- Patients in the observation group who crossed over to receive VIDAZA treatment (47 patients) had a response rate of 12.8%. Study 2, a multi-center, open-label, single-arm study of 72 patients with RAEB, RAEB-T, CMMoL, or AML was also carried out. Treatment with subcutaneous VIDAZA resulted in a response rate (CR + PR) of 13.9%, using criteria similar to those described above. The mean and median duration of clinical response of PR or better was estimated as 810 and 430 days, respectively; 80% of the responding patients were still in PR or better at the time of completion of study involvement. In Study 3, another open-label, single-arm study of 48 patients with RAEB, RAEB-T, or AML, treatment with intravenous VIDAZA resulted in a response rate of 18.8%, again using criteria similar to those described above. The mean and median duration of clinical response of PR or better was estimated as 389 and 281 days, respectively; 67% of the responding patients were still in PR or better at the time of completion of treatment. Response occurred in all MDS subtypes as well as in patients with adjudicated baseline diagnosis of AML in both of these studies. VIDAZA dosage regimens in these 2 studies were similar to the regimen used in the controlled study. Benefit was seen in patients who did not meet the criteria for PR or better, but were considered “improved.” About 24% of VIDAZA-treated patients were considered improved, and about 2/3 of those lost transfusion dependence. In the observation group, only 5/83 patients met criteria for improvement; none lost transfusion dependence. In all 3 studies, about 19% of patients met criteria for improvement with a median duration of 195 days. Study 4 was an international, multicenter, open-label, randomized trial in patients with MDS with RAEB, RAEB-T or modified CMMoL according to FAB classification and Intermediate-2 and High risk according to IPSS classification. Of the 358 patients enrolled in the study, 179 were randomized to receive azacitidine plus best supportive care (BSC) and 179 were randomized to receive conventional care regimens (CCR) plus BSC (105 to BSC alone, 49 to low dose cytarabine and 25 to chemotherapy with cytarabine and anthracycline). The primary efficacy endpoint was overall survival. The azacitidine and CCR groups were comparable for baseline parameters. The median age of patients was 69 years (range was 38-88 years), 98% were Caucasian, and 70% were male. At baseline, 95% of the patients were higher risk by FAB classification: RAEB (58%), RAEB-T (34%), and CMMoL (3%). By IPSS classification, 87% were higher risk: Int-2 (41%), High (47%). At baseline, 32% of patients met WHO criteria for AML. Azacitidine was administered subcutaneously at a dose of 75 mg/m 2 daily for 7 consecutive days every 28 days (which constituted one cycle of therapy). Patients continued treatment until disease progression, relapse after response, or unacceptable toxicity. Azacitidine patients were treated for a median of 9 cycles (range 1 to 39), BSC only patients for a median of 7 cycles (range 1 to 26), low dose cytarabine patients for a median of 4.5 cycles (range 1 to 15), and chemotherapy with cytarabine and anthracycline patients for a median of 1 cycle (range 1 to 3, i.e. induction plus 1 or 2 consolidation cycles). In the Intent-to-Treat analysis, patients treated with azacitidine demonstrated a statistically significant difference in overall survival as compared to patients treated with CCR (median survival of 24.5 months vs. 15.0 months; stratified log-rank p=0.0001). The hazard ratio describing this treatment effect was 0.58 (95% CI: 0.43, 0.77). Kaplan-Meier Curve of Time to Death from Any Cause: (Intent-to-Treat Population) Key: AZA = azacitidine; CCR = conventional care regimens; CI = confidence interval; HR = Hazard Ratio Azacitidine treatment led to a reduced need for red blood cell transfusions (see Table 8). In patients treated with azacitidine who were RBC transfusion dependent at baseline and became transfusion independent, the median duration of RBC transfusion independence was 13.0 months. Table 9. Effect of Azacitidine on RBC Transfusions in Patients with MDS Efficacy Parameter Azacitidine plus BSC (n= 179) Conventional Care Regimens (n= 179) Number and percent of patients who were transfusion dependent at baseline who became transfusion independent on treatment 1 50/111 (45.0%) 13/114 (11.4%) (95% CI: 35.6%, 54.8%) (95% CI: 6.2%, 18.7%) Number and percent of patients who were transfusion-independent at baseline who became transfusion-dependent on treatment 10/68 (14.7%) 28/65 (43.1%) (95% CI: 7.3%, 25.4%) (95% CI: 30.9%, 56.0%) 1 A patient was considered RBC transfusion independent during the treatment period if the patient had no RBC transfusions during any 56 consecutive days or more during the treatment period. Otherwise, the patient was considered transfusion dependent. Kaplan-Meier Curve of Time to Death from Any Cause: (Intent-to-Treat Population) 14.2 Juvenile Myelomonocytic Leukemia (JMML) AZA-JMML-001 (NCT02447666) was an international, multicenter, open-label study to evaluate the pharmacokinetics, pharmacodynamics, safety, and activity of VIDAZA prior to hematopoietic stem cell transplantation (HSCT) in a total of 18 pediatric patients (median age of 2.1 years, range 0.2-6.9 years; 61% male; 89% white) with juvenile myelomonocytic leukemia (JMML). Patients with newly diagnosed JMML were included if they met the following criteria: diagnosis confirmed in peripheral blood and bone marrow, and had one of the following: somatic mutation in PTPN11, KRAS, or NRAS and HbF % > 5 x normal value for age, or clinical diagnosis of neurofibromatosis Type 1 (NF-1). Additionally, patients included had no CNS involvement, isolated extramedullary disease, or germline molecular aberrations in CBL, PTPN11, NRAS, or KRAS. Eighteen patients with JMML (13 PTPN11 , 3 NRAS , 1 KRAS somatic mutations and 1 clinical diagnosis of neurofibromatosis type 1 [ NF 1 ]) were enrolled. Patients were treated with intravenous VIDAZA [see Dosage and Administration ( 2.4 )] , daily on Days 1 to 7 of a 28-day cycle for a minimum of 3 cycles and a maximum of 6 cycles, provided the patients did not have disease progression or were ready for HSCT between Cycles 4 and 6. The efficacy of VIDAZA was established based on clinical complete remission (cCR) or clinical partial remission (cPR) according to the International JMML response criteria at 3 months (Cycle 3 Day 28). Responses must have been sustained for at least 4 weeks either in the 4-week period preceding or succeeding Cycle 3 Day 28 (i.e., sustained over the period Cycle 2 Day 28 to Cycle 3 Day 28, or Cycle 3 Day 28 to Cycle 4 Day 28). There were a total of 9 patients (50%, 95% CI 26-74) with a confirmed clinical response. Of these 9 patients, there were 3 cCR and 6 cPR. The median time to response was 1.2 months (range 1-1.9 months). The proportion of patients with JMML undergoing HSCT was 94% and the median time to HSCT was 4.6 months (range 2.8-19 months).

Clinical Studies Table

VIDAZA (N=99)Observation (N=92)

Gender (n%)

Male

72 (72.7)

60 (65.2)

Female

27 (27.3)

32 (34.8)

Race (n%)

White

93 (93.9)

85 (92.4)

Black

1 (1.0)

1 (1.1)

Hispanic

3 (3.0)

5 (5.4)

Asian/Oriental

2 (2.0)

1 (1.1)

Age (years)

N

99

91

Mean ± SD

67.3 ± 10.39

68.0 ± 10.23

Range

31 - 92

35 - 88

Adjudicated MDS diagnosis at study entry (n%)

RA

21 (21.2)

18 (19.6)

RARS

6 (6.1)

5 (5.4)

RAEB

38 (38.4)

39 (42.4)

RAEB-T

16 (16.2)

14 (15.2)

CMMoL

8 (8.1)

7 (7.6)

AML

10 (10.1)

9 (9.8)

Transfusion product used in 3 months before study entry (n%)

Any transfusion product

70 (70.7)

59 (64.1)

Blood cells, packed human

66 (66.7)

55 (59.8)

Platelets, human blood

15 (15.2)

12 (13.0)

Hetastarch

0(0.0)

1(1.1)

Plasma protein fraction

1(1.0)

0(0.0)

Other

2(2.0)

2(2.2)

References

15 REFERENCES 1. “OSHA Hazardous Drugs.” OSHA. http://www.osha.gov/SLTC/hazardousdrugs/index.html

Geriatric Use

8.5 Geriatric Use Of the total number of patients in Studies 1, 2 and 3, 62% were 65 years and older and 21% were 75 years and older. No overall differences in effectiveness were observed between these patients and younger patients. In addition, there were no relevant differences in the frequency of adverse reactions observed in patients 65 years and older compared to younger patients. Of the 179 patients randomized to azacitidine in Study 4, 68% were 65 years and older and 21% were 75 years and older. Survival data for patients 65 years and older were consistent with overall survival results. The majority of adverse reactions occurred at similar frequencies in patients <65 years of age and patients 65 years of age and older. Elderly patients are more likely to have decreased renal function. Monitor renal function in these patients [see Dosage and Administration ( 2.7 ) and Warnings and Precautions ( 5.4 )].

Pediatric Use

8.4 Pediatric Use Safety and effectiveness of VIDAZA in pediatric patients with MDS have not been established. The safety and effectiveness of VIDAZA have been established in pediatric patients with newly diagnosed JMML aged 1 month and older and the information on this use is discussed throughout the labeling. The safety and effectiveness of VIDAZA have not been established in pediatric patients younger than 1 month old [see Clinical Studies ( 14.2 )] .

Pregnancy

8.1 Pregnancy Risk Summary Based on its mechanism of action and findings in animals, VIDAZA can cause fetal harm when administered to a pregnant woman [see Clinical Pharmacology ( 12.1 )]. There are no data on the use of azacitidine in pregnant women. Azacitidine was teratogenic and caused embryo-fetal lethality in animals at doses lower than the recommended human daily dose (see Data). Advise pregnant women of the potential risk to the fetus. The background rate of major birth defects and miscarriage is unknown for the indicated population. All pregnancies have a background risk of birth defect, loss, or other adverse outcomes. In the U.S. general population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2%-4% and 15%-20%, respectively. Data Animal Data Early embryotoxicity studies in mice revealed a 44% frequency of intrauterine embryonal death (increased resorption) after a single IP (intraperitoneal) injection of 6 mg/m 2 (approximately 8% of the recommended human daily dose on a mg/m 2 basis) azacitidine on gestation day 10. Developmental abnormalities in the brain have been detected in mice given azacitidine on or before gestation day 15 at doses of ~3-12 mg/m 2 (approximately 4%-16% the recommended human daily dose on a mg/m 2 basis). In rats, azacitidine was clearly embryotoxic when given IP on gestation days 4-8 (postimplantation) at a dose of 6 mg/m 2 (approximately 8% of the recommended human daily dose on a mg/m 2 basis), although treatment in the preimplantation period (on gestation days 1-3) had no adverse effect on the embryos. Azacitidine caused multiple fetal abnormalities in rats after a single IP dose of 3 to 12 mg/m 2 (approximately 8% the recommended human daily dose on a mg/m 2 basis) given on gestation day 9, 10, 11 or 12. In this study azacitidine caused fetal death when administered at 3-12 mg/m 2 on gestation days 9 and 10; average live animals per litter was reduced to 9% of control at the highest dose on gestation day 9. Fetal anomalies included: CNS anomalies (exencephaly/encephalocele), limb anomalies (micromelia, club foot, syndactyly, oligodactyly), and others (micrognathia, gastroschisis, edema, and rib abnormalities).

Use In Specific Populations

8 USE IN SPECIFIC POPULATIONS • Lactation: Advise not to breastfeed ( 8.2 ). 8.1 Pregnancy Risk Summary Based on its mechanism of action and findings in animals, VIDAZA can cause fetal harm when administered to a pregnant woman [see Clinical Pharmacology ( 12.1 )]. There are no data on the use of azacitidine in pregnant women. Azacitidine was teratogenic and caused embryo-fetal lethality in animals at doses lower than the recommended human daily dose (see Data). Advise pregnant women of the potential risk to the fetus. The background rate of major birth defects and miscarriage is unknown for the indicated population. All pregnancies have a background risk of birth defect, loss, or other adverse outcomes. In the U.S. general population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2%-4% and 15%-20%, respectively. Data Animal Data Early embryotoxicity studies in mice revealed a 44% frequency of intrauterine embryonal death (increased resorption) after a single IP (intraperitoneal) injection of 6 mg/m 2 (approximately 8% of the recommended human daily dose on a mg/m 2 basis) azacitidine on gestation day 10. Developmental abnormalities in the brain have been detected in mice given azacitidine on or before gestation day 15 at doses of ~3-12 mg/m 2 (approximately 4%-16% the recommended human daily dose on a mg/m 2 basis). In rats, azacitidine was clearly embryotoxic when given IP on gestation days 4-8 (postimplantation) at a dose of 6 mg/m 2 (approximately 8% of the recommended human daily dose on a mg/m 2 basis), although treatment in the preimplantation period (on gestation days 1-3) had no adverse effect on the embryos. Azacitidine caused multiple fetal abnormalities in rats after a single IP dose of 3 to 12 mg/m 2 (approximately 8% the recommended human daily dose on a mg/m 2 basis) given on gestation day 9, 10, 11 or 12. In this study azacitidine caused fetal death when administered at 3-12 mg/m 2 on gestation days 9 and 10; average live animals per litter was reduced to 9% of control at the highest dose on gestation day 9. Fetal anomalies included: CNS anomalies (exencephaly/encephalocele), limb anomalies (micromelia, club foot, syndactyly, oligodactyly), and others (micrognathia, gastroschisis, edema, and rib abnormalities). 8.2 Lactation Risk Summary There is no information regarding the presence of azacitidine in human milk, the effects of VIDAZA on the breastfed infant, or the effects of VIDAZA on milk production. Because many drugs are excreted in human milk and because of the potential for tumorigenicity shown for azacitidine in animal studies [see Nonclinical Toxicology ( 13.1 )] and the potential for serious adverse reactions in nursing infants from VIDAZA, advise patients not to breastfeed during treatment with VIDAZA and for 1 week after the last dose. 8.3 Females and Males of Reproductive Potential Based on its mechanism of action and findings in animals, VIDAZA can cause fetal harm when administered to a pregnant woman [see Use in Specific Populations ( 8.1 )]. Pregnancy Testing Verify the pregnancy status of females of reproductive potential prior to initiating VIDAZA. Contraception Females Advise pregnant women of the potential risk to a fetus. Advise females of reproductive potential to use effective contraception during treatment with VIDAZA and for 6 months after the last dose. Males Advise males with female partners of reproductive potential to use effective contraception during treatment with VIDAZA and for 3 months after the last dose. Infertility Based on animal data, azacitidine could have an effect on male or female fertility [see Nonclinical Toxicology ( 13.1 )]. 8.4 Pediatric Use Safety and effectiveness of VIDAZA in pediatric patients with MDS have not been established. The safety and effectiveness of VIDAZA have been established in pediatric patients with newly diagnosed JMML aged 1 month and older and the information on this use is discussed throughout the labeling. The safety and effectiveness of VIDAZA have not been established in pediatric patients younger than 1 month old [see Clinical Studies ( 14.2 )] . 8.5 Geriatric Use Of the total number of patients in Studies 1, 2 and 3, 62% were 65 years and older and 21% were 75 years and older. No overall differences in effectiveness were observed between these patients and younger patients. In addition, there were no relevant differences in the frequency of adverse reactions observed in patients 65 years and older compared to younger patients. Of the 179 patients randomized to azacitidine in Study 4, 68% were 65 years and older and 21% were 75 years and older. Survival data for patients 65 years and older were consistent with overall survival results. The majority of adverse reactions occurred at similar frequencies in patients <65 years of age and patients 65 years of age and older. Elderly patients are more likely to have decreased renal function. Monitor renal function in these patients [see Dosage and Administration ( 2.7 ) and Warnings and Precautions ( 5.4 )].

How Supplied

16 HOW SUPPLIED/STORAGE AND HANDLING How Supplied VIDAZA (azacitidine for injection) is supplied as a lyophilized powder in 100 mg single-dose vials packaged in cartons of 1 vial (NDC 59572-102-01). Storage Store unreconstituted vials at 25º C (77º F); excursions permitted to 15º-30º C (59º-86º F) (See USP Controlled Room Temperature). Handling and Disposal VIDAZA is a hazardous drug. Follow applicable special handling and disposal procedures. 1

Storage And Handling

Storage Store unreconstituted vials at 25º C (77º F); excursions permitted to 15º-30º C (59º-86º F) (See USP Controlled Room Temperature).

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