Adults
Osteoarthritis and Rheumatoid Arthritis
The meloxicam Phase 2/3 clinical trial database includes 10,122 OA patients and 1012 RA patients treated with meloxicam 7.5 mg/day, 3505 OA patients and 1351 RA patients treated with meloxicam 15 mg/day. Meloxicam at these doses was administered to 661 patients for at least 6 months and to 312 patients for at least one year. Approximately 10,500 of these patients were treated in ten placebo- and/or active-controlled osteoarthritis trials and 2363 of these patients were treated in ten placebo- and/or active-controlled rheumatoid arthritis trials. Gastrointestinal (GI) adverse events were the most frequently reported adverse events in all treatment groups across meloxicam trials.
A 12-week multicenter, double-blind, randomized trial was conducted in patients with osteoarthritis of the knee or hip to compare the efficacy and safety of meloxicam with placebo and with an active control. Two 12-week multicenter, double-blind, randomized trials were conducted in patients with rheumatoid arthritis to compare the efficacy and safety of meloxicam with placebo.
Table 1a depicts adverse events that occurred in ≥2% of the meloxicam treatment groups in a 12-week placebo- and active-controlled osteoarthritis trial.
Table 1b depicts adverse events that occurred in ≥2% of the meloxicam treatment groups in two 12-week placebo- controlled rheumatoid arthritis trials.
Table 1a Adverse Events (%) Occurring in ≥2% of Meloxicam Patients in a 12-Week Osteoarthritis Placebo- and Active-Controlled Trial
|
| Placebo | Meloxicam
7.5 mg daily | Meloxicam
15 mg daily | Diclofenac
100 mg daily |
| No. of Patients | 157 | 154 | 156 | 153 |
| Gastrointestinal | 17.2
| 20.1
| 17.3
| 28.1
|
| Abdominal Pain
| 2.5
| 1.9
| 2.6
| 1.3
|
| Diarrhea
| 3.8
| 7.8
| 3.2
| 9.2
|
| Dyspepsia
| 4.5
| 4.5
| 4.5
| 6.5
|
| Flatulence
| 4.5
| 3.2
| 3.2
| 3.9
|
| Nausea
| 3.2
| 3.9
| 3.8
| 7.2
|
| Body as a Whole | | | | |
| Accident Household
| 1.9
| 4.5
| 3.2
| 2.6
|
| Edema1 | 2.5
| 1.9
| 4.5
| 3.3
|
| Fall
| 0.6
| 2.6
| 0.0
| 1.3
|
| Influenza-Like Symptoms
| 5.1
| 4.5
| 5.8
| 2.6
|
| Central and Peripheral Nervous System | | | | |
| Dizziness
| 3.2
| 2.6
| 3.8
| 2.0
|
| Headache
| 10.2
| 7.8
| 8.3
| 5.9
|
| Respiratory | | | | |
| Pharyngitis
| 1.3
| 0.6
| 3.2
| 1.3
|
| Upper Respiratory Tract Infection
| 1.9
| 3.2
| 1.9
| 3.3
|
| Skin | | | | |
| Rash2 | 2.5
| 2.6
| 0.6
| 2.0
|
Table 1b Adverse Events (%) Occurring in ≥2% of Meloxicam Patients in two 12-Week Rheumatoid Arthritis Placebo-Controlled Trials
|
| Placebo | Meloxicam
7.5 mg daily | Meloxicam
15 mg daily |
| No. of Patients | 469 | 481 | 477 |
| Gastrointestinal Disorders | 14.1
| 18.9
| 16.8
|
| Abdominal Pain NOS2 | 0.6
| 2.9
| 2.3
|
| Dyspeptic signs and symptoms1 | 3.8
| 5.8
| 4.0
|
| Nausea2 | 2.6
| 3.3
| 3.8
|
| General Disorders and Administration Site Conditions |
| Influenza like illness2 | 2.1
| 2.9
| 2.3
|
| Infection and Infestations |
| Upper respiratory tract infections-pathogen class unspecified1 | 4.1
| 7.0
| 6.5
|
| Musculoskeletal and Connective Tissue Disorders |
| Joint related signs and symptoms1 | 1.9
| 1.5
| 2.3
|
| | | |
| Nervous System Disorders | | | |
| Headaches NOS2 | 6.4
| 6.4
| 5.5
|
| | | |
| Skin and Subcutaneous Tissue Disorders |
| Rash NOS2 | 1.7
| 1.0
| 2.1
|
The adverse events that occurred with meloxicam in ≥ 2% of patients treated short-term (4 to 6 weeks) and long-term (6 months) in active-controlled osteoarthritis trials are presented in Table 2.
Table 2 Adverse Events (%) Occurring in ≥2% of Meloxicam Patients in 4 to 6 Weeks and 6 Month Active-Controlled Osteoarthritis Trials
|
| 4 to 6 Weeks Controlled Trials | 6 Month Controlled Trials |
| Meloxicam
7.5 mg daily | Meloxicam
15 mg daily | Meloxicam
7.5 mg daily | Meloxicam
15 mg daily |
| No. of Patients | 8955 | 256 | 169 | 306 |
| Gastrointestinal | 11.8
| 18.0
| 26.6
| 24.2
|
| Abdominal Pain
| 2.7
| 2.3
| 4.7
| 2.9
|
| Constipation
| 0.8
| 1.2
| 1.8
| 2.6
|
| Diarrhea
| 1.9
| 2.7
| 5.9
| 2.6
|
| Dyspepsia
| 3.8
| 7.4
| 8.9
| 9.5
|
| Flatulence
| 0.5
| 0.4
| 3.0
| 2.6
|
| Nausea
| 2.4
| 4.7
| 4.7
| 7.2
|
| Vomiting
| 0.6
| 0.8
| 1.8
| 2.6
|
| Body as a Whole | | | | |
| Accident Household
| 0.0
| 0.0
| 0.6
| 2.9
|
| Edema1 | 0.6
| 2.0
| 2.4
| 1.6
|
| Pain
| 0.9
| 2.0
| 3.6
| 5.2
|
| Central and Peripheral Nervous System |
| Dizziness
| 1.1
| 1.6
| 2.4
| 2.6
|
| Headache
| 2.4
| 2.7
| 3.6
| 2.6
|
| Hematologic | | | | |
| Anemia
| 0.1
| 0.0
| 4.1
| 2.9
|
| Musculoskeletal | | | | |
| Arthralgia
| 0.5
| 0.0
| 5.3
| 1.3
|
| Back Pain
| 0.5
| 0.4
| 3.0
| 0.7
|
| Psychiatric | | | | |
| Insomnia
| 0.4
| 0.0
| 3.6
| 1.6
|
| Respiratory | | | | |
| Coughing
| 0.2
| 0.8
| 2.4
| 1.0
|
| Upper Respiratory Tract Infection
| 0.2
| 0.0
| 8.3
| 7.5
|
| Skin | | | | |
| Pruritus
| 0.4
| 1.2
| 2.4
| 0.0
|
| Rash2 | 0.3
| 1.2
| 3.0
| 1.3
|
| Urinary | | | | |
| Micturition Frequency
| 0.1
| 0.4
| 2.4
| 1.3
|
| Urinary Tract Infection
| 0.3
| 0.4
| 4.7
| 6.9
|
Higher doses of meloxicam (22.5 mg and greater) have been associated with an increased risk of serious GI events; therefore the daily dose of meloxicam should not exceed 15 mg.
The following is a list of adverse drug reactions occurring in < 2% of patients receiving meloxicam in clinical trials involving approximately 16,200 patients.
| Body as a Whole | allergic reaction, face edema, fatigue, fever, hot flushes, malaise, syncope, weight decrease, weight increase
|
| Cardiovascular | angina pectoris, cardiac failure, hypertension, hypotension, myocardial infarction, vasculitis
|
| Central and Peripheral Nervous System | convulsions, paresthesia, tremor, vertigo
|
| Gastrointestinal | colitis, dry mouth, duodenal ulcer, eructation, esophagitis, gastric ulcer, gastritis, gastroesophageal reflux, gastrointestinal hemorrhage, hematemesis, hemorrhagic duodenal ulcer, hemorrhagic gastric ulcer, intestinal perforation, melena, pancreatitis, perforated duodenal ulcer, perforated gastric ulcer, stomatitis ulcerative
|
| Heart Rate and Rhythm | arrhythmia, palpitation, tachycardia
|
| Hematologic | leukopenia, purpura, thrombocytopenia
|
| Liver and Biliary System | ALT increased, AST increased, bilirubinemia, GGT increased, hepatitis
|
| Metabolic and Nutritional | dehydration
|
Psychiatric
| abnormal dreaming, anxiety, appetite increased, confusion, depression, nervousness, somnolence
|
| Respiratory | asthma, bronchospasm, dyspnea
|
| Skin and Appendages | alopecia, angioedema, bullous eruption, photosensitivity reaction, pruritus, sweating increased, urticaria
|
| Special Senses | abnormal vision, conjunctivitis, taste perversion, tinnitus
|
| Urinary System | albuminuria, BUN increased, creatinine increased, hematuria, renal failure
|
Pregnancy Category C; Category D starting 30 weeks gestation
There are no adequate and well-controlled studies in pregnant women. Meloxicam crosses the placental barrier. Prior to 30 weeks gestation, use meloxicam during pregnancy only if the potential benefit justifies the potential risk to the fetus. Starting at 30 weeks gestation, avoid meloxicam and other NSAIDs, in pregnant women as premature closure of the ductus arteriosus in the fetus may occur. If this drug is used during this time period in pregnancy, inform the patient of the potential hazard to a fetus [see Warnings and Precautions (5.9) and Patient Counseling Information (17.8)].
Absorption
The absolute bioavailability of meloxicam capsules was 89% following a single oral dose of 30 mg compared with 30 mg IV bolus injection. Following single intravenous doses, dose-proportional pharmacokinetics were shown in the range of 5 mg to 60 mg. After multiple oral doses the pharmacokinetics of meloxicam capsules were dose-proportional over the range of 7.5 mg to 15 mg. Mean Cmax was achieved within four to five hours after a 7.5 mg meloxicam tablet was taken under fasted conditions, indicating a prolonged drug absorption. With multiple dosing, steady-state concentrations were reached by Day 5. A second meloxicam concentration peak occurs around 12 to 14 hours post-dose suggesting biliary recycling.
Table 3 Single Dose and Steady-State Pharmacokinetic Parameters for Oral 7.5 mg and 15 mg Meloxicam (Mean and % CV)1 |
| Steady State | Single Dose |
Pharmacokinetic Parameters
(% CV) | Healthy male adults
(Fed)2 | Elderly males
(Fed)2 | Elderly females (Fed)2 | Renal failure (Fasted) | Hepatic insufficiency
(Fasted) |
| 7.5 mg3
tablets | 15 mg capsules | 15 mg capsules | 15 mg capsules | 15 mg capsules |
| N | 18 | 5 | 8 | 12 | 12 |
| Cmax | [mcg/mL]
| 1.05 (20)
| 2.3 (59)
| 3.2 (24)
| 0.59 (36)
| 0.84 (29)
|
| tmax | [h]
| 4.9 (8)
| 5 (12)
| 6 (27)
| 4 (65)
| 10 (87)
|
| t1/2 | [h]
| 20.1 (29)
| 21 (34)
| 24 (34)
| 18 (46)
| 16 (29)
|
| CL/f
| [mL/min]
| 8.8 (29)
| 9.9 (76)
| 5.1 (22)
| 19 (43)
| 11 (44)
|
| Vz/f4 | [L]
| 14.7 (32)
| 15 (42)
| 10 (30)
| 26 (44)
| 14 (29)
|
Food and Antacid Effects
Administration of meloxicam capsules following a high fat breakfast (75 g of fat) resulted in mean peak drug levels (i.e., Cmax) being increased by approximately 22% while the extent of absorption (AUC) was unchanged. The time to maximum concentration (Tmax) was achieved between 5 and 6 hours. In comparison, neither the AUC nor the Cmax values for meloxicam suspension were affected following a similar high fat meal, while mean Tmax values were increased to approximately 7 hours. No pharmacokinetic interaction was detected with concomitant administration of antacids. Based on these results, meloxicam can be administered without regard to timing of meals or concomitant administration of antacids.
Distribution
The mean volume of distribution (Vss) of meloxicam is approximately 10 L. Meloxicam is ~99.4% bound to human plasma proteins (primarily albumin) within the therapeutic dose range. The fraction of protein binding is independent of drug concentration, over the clinically relevant concentration range, but decreases to ~99% in patients with renal disease. Meloxicam penetration into human red blood cells, after oral dosing, is less than 10%. Following a radiolabeled dose, over 90% of the radioactivity detected in the plasma was present as unchanged meloxicam.
Meloxicam concentrations in synovial fluid, after a single oral dose, range from 40% to 50% of those in plasma. The free fraction in synovial fluid is 2.5 times higher than in plasma, due to the lower albumin content in synovial fluid as compared to plasma. The significance of this penetration is unknown.
Metabolism
Meloxicam is extensively metabolized in the liver. Meloxicam metabolites include 5'-carboxy meloxicam (60% of dose), from P-450 mediated metabolism formed by oxidation of an intermediate metabolite 5'-hydroxymethyl meloxicam which is also excreted to a lesser extent (9% of dose). In vitro studies indicate that CYP2C9 (cytochrome P450 metabolizing enzyme) plays an important role in this metabolic pathway with a minor contribution of the CYP3A4 isozyme. Patients' peroxidase activity is probably responsible for the other two metabolites which account for 16% and 4% of the administered dose, respectively. All the four metabolites are not known to have any in vivo pharmacological activity.
Excretion
Meloxicam excretion is predominantly in the form of metabolites, and occurs to equal extents in the urine and feces. Only traces of the unchanged parent compound are excreted in the urine (0.2%) and feces (1.6%). The extent of the urinary excretion was confirmed for unlabeled multiple 7.5 mg doses: 0.5%, 6%, and 13% of the dose were found in urine in the form of meloxicam, and the 5'-hydroxymethyl and 5'-carboxy metabolites, respectively. There is significant biliary and/or enteral secretion of the drug. This was demonstrated when oral administration of cholestyramine following a single IV dose of meloxicam decreased the AUC of meloxicam by 50%.
The mean elimination half-life (t1/2) ranges from 15 hours to 20 hours. The elimination half-life is constant across dose levels indicating linear metabolism within the therapeutic dose range. Plasma clearance ranges from 7 to 9 mL/min.
Special Populations
Pediatric
After single (0.25 mg/kg) dose administration and after achieving steady state (0.375 mg/kg/day), there was a general trend of approximately 30% lower exposure in younger patients (2 to 6 years old) as compared to the older patients (7 to 16 years old). The older patients had meloxicam exposures similar (single dose) or slightly reduced (steady state) to those in the adult patients, when using AUC values normalized to a dose of
0.25 mg/kg [see Dosage and Administration (2.4)]. The meloxicam mean (SD) elimination half-life was 15.2 (10.1) and 13.0 hours (3.0) for the 2 to 6 year old patients, and 7 to 16 year old patients, respectively.
In a covariate analysis, utilizing population pharmacokinetics body-weight, but not age, was the single predictive covariate for differences in the meloxicam apparent oral plasma clearance. The body-weight normalized apparent oral clearance values were adequate predictors of meloxicam exposure in pediatric patients.
The pharmacokinetics of meloxicam in pediatric patients under 2 years of age have not been investigated.
Geriatric
Elderly males (≥65 years of age) exhibited meloxicam plasma concentrations and steady-state pharmacokinetics similar to young males. Elderly females (≥65 years of age) had a 47% higher AUCss and 32% higher Cmax,ss as compared to younger females (≤55 years of age) after body weight normalization. Despite the increased total concentrations in the elderly females, the adverse event profile was comparable for both elderly patient populations. A smaller free fraction was found in elderly female patients in comparison to elderly male patients.
Gender
Young females exhibited slightly lower plasma concentrations relative to young males. After single doses of 7.5 mg meloxicam, the mean elimination half-life was 19.5 hours for the female group as compared to 23.4 hours for the male group. At steady state, the data were similar
(17.9 hours vs 21.4 hours). This pharmacokinetic difference due to gender is likely to be of little clinical importance. There was linearity of pharmacokinetics and no appreciable difference in the Cmax or Tmax across genders.
Hepatic Impairment
Following a single 15 mg dose of meloxicam there was no marked difference in plasma concentrations in patients with mild (Child-Pugh Class I) or moderate (Child-Pugh Class II) hepatic impairment compared to healthy volunteers. Protein binding of meloxicam was not affected by hepatic impairment. No dosage adjustment is necessary in patients with mild to moderate hepatic impairment. Patients with severe hepatic impairment (Child-Pugh Class III) have not been adequately studied [see Warnings and Precautions (5.3) and Use in Specific Populations (8.6)].
Renal Impairment
Meloxicam pharmacokinetics have been investigated in subjects with mild and moderate renal impairment. Total drug plasma concentrations of meloxicam decreased and total clearance of meloxicam increased with the degree of renal impairment while free AUC values were similar in all groups. The higher meloxicam clearance in subjects with renal impairment may be due to increased fraction of unbound meloxicam which is available for hepatic metabolism and subsequent excretion. No dosage adjustment is necessary in patients with mild to moderate renal impairment. Patients with severe renal impairment have not been adequately studied. The use of meloxicam in subjects with severe renal impairment is not recommended [see Warnings and Precautions (5.6) and Use in Specific Populations (8.7)].
Hemodialysis
Following a single dose of meloxicam, the free Cmax plasma concentrations were higher in patients with renal failure on chronic hemodialysis (1% free fraction) in comparison to healthy volunteers (0.3% free fraction). Hemodialysis did not lower the total drug concentration in plasma; therefore, additional doses are not necessary after hemodialysis. Meloxicam is not dialyzable [see Dosage and Administration (2.1), Warnings and Precautions (5.6), and Use in Specific Populations (8.7)].
Drug Interactions
Aspirin: When meloxicam is administered with aspirin (1000 mg three times daily) to healthy volunteers, it tended to increase the AUC (10%) and Cmax (24%) of meloxicam. The clinical significance of this interaction is not known [see Drug Interactions (7.2)].
Cholestyramine: Pretreatment for four days with cholestyramine significantly increased the clearance of meloxicam by 50%. This resulted in a decrease in t1/2, from 19.2 hours to 12.5 hours, and a 35% reduction in AUC. This suggests the existence of a recirculation pathway for meloxicam in the gastrointestinal tract. The clinical relevance of this interaction has not been established.
Cimetidine: Concomitant administration of 200 mg cimetidine four times daily did not alter the single-dose pharmacokinetics of 30 mg meloxicam.
Digoxin: Meloxicam 15 mg once daily for 7 days did not alter the plasma concentration profile of digoxin after β-acetyldigoxin administration for 7 days at clinical doses. In vitro testing found no protein binding drug interaction between digoxin and meloxicam.
Lithium: In a study conducted in healthy subjects, mean pre-dose lithium concentration and AUC were increased by 21% in subjects receiving lithium doses ranging from 804 to 1072 mg twice daily with meloxicam 15 mg QD every day as compared to subjects receiving lithium alone [see Drug Interactions (7.4)].
Methotrexate: A study in 13 rheumatoid arthritis (RA) patients evaluated the effects of multiple doses of meloxicam on the pharmacokinetics of methotrexate taken once weekly. Meloxicam did not have a significant effect on the pharmacokinetics of single doses of methotrexate. In vitro, methotrexate did not displace meloxicam from its human serum binding sites [see Drug Interactions (7.5)].
Warfarin: The effect of meloxicam on the anticoagulant effect of warfarin was studied in a group of healthy subjects receiving daily doses of warfarin that produced an INR (International Normalized Ratio) between 1.2 and 1.8. In these subjects, meloxicam did not alter warfarin pharmacokinetics and the average anticoagulant effect of warfarin as determined by prothrombin time. However, one subject showed an increase in INR from 1.5 to 2.1. Caution should be used when administering meloxicam with warfarin since patients on warfarin may experience changes in INR and an increased risk of bleeding complications when a new medication is introduced [see Drug Interactions (7.7)].
Carcinogenesis: There was no increase in tumor incidence in long-term carcinogenicity studies in rats (104 weeks) and mice (99 weeks) administered meloxicam at oral doses up to 0.8 mg/kg/day in rats and up to 8.0 mg/kg/day in mice (up to 0.5- and 2.6-fold, respectively, the maximum recommended human daily dose based on body surface area comparison).
Mutagenesis: Meloxicam was not mutagenic in an Ames assay, or clastogenic in a chromosome aberration assay with human lymphocytes and an in vivo micronucleus test in mouse bone marrow.
Impairment of Fertility: Meloxicam did not impair male and female fertility in rats at oral doses up to 9 mg/kg/day in males and 5 mg/kg/day in females (up to 5.8- and 3.2-fold greater, respectively, than the maximum recommended human daily dose based on body surface area comparison).
