result in decreased exposure of carisoprodol and increased exposure of meprobamate. low dose aspirin also showed an induction effect on cyp2c19. the full pharmacological impact of these potential alterations of exposures in terms of either efficacy or safety of carisoprodol is unknown.

ercised with patients who take more than one of these cns depressants simultaneously. 5.2 abuse, dependence and withdrawal carisoprodol, the active ingredient in carisoprodol, has been subject to abuse, dependence, and withdrawal, misuse and criminal diversion [see drug abuse and dependence ( 9.1 , 9.2 , 9.3) ]. abuse of carisoprodol poses a risk of overdosage which may lead to death, cns and respiratory depression, hypotension, seizures and other disorders [see overdosage (10) ]. post-marketing experience cases of carisoprodol abuse and dependence have been reported in patients with prolonged use and a history of drug abuse. although most of these patients took other drugs of abuse, some patients solely abused carisoprodol. withdrawal symptoms have been reported following abrupt cessation of carisoprodol after prolonged use. reported withdrawal symptoms included insomnia, vomiting, abdominal cramps, headache, tremors, muscle twitching, ataxia, hallucinations, and psychosis. one of carisoprodol’s metabolites, meprobamate (a controlled substance), may also cause dependence [see clinical pharmacology (12.3) ]. to reduce the risk of carisoprodol abuse assess the risk of abuse prior to prescribing. after prescribing, limit the length of treatment to three weeks for the relief of acute musculoskeletal discomfort, keep careful prescription records, monitor for signs of abuse and overdose, and educate patients and their families about abuse and on proper storage and disposal. 5.3 seizures there have been post-marketing reports of seizures in patients who received carisoprodol. most of these cases have occurred in the setting of multiple drug overdoses (including drugs of abuse, illegal drugs, and alcohol) [see overdosage (10) ].

d 74% caucasian, 16% black, 9% asian, and 2% other. there were no deaths and there were no serious adverse reactions in these two trials. in these two studies, 2.7%, 2%, and 5.4%, of patients treated with placebo, 250 mg of carisoprodol, and 350 mg of carisoprodol, respectively, discontinued due to adverse events; and 0.5%, 0.5%, and 1.8% of patients treated with placebo, 250 mg of carisoprodol, and 350 mg of carisoprodol, respectively, discontinued due to central nervous system adverse reactions. table 1 displays adverse reactions reported with frequencies greater than 2% and more frequently than placebo in patients treated with carisoprodol in the two trials described above. table 1. patients with adverse reactions in controlled studies adverse reaction placebo (n=560) n (%) carisoprodol 250 mg (n=548) n (%) carisoprodol 350 mg (n=279) n (%) drowsiness 31 (6) 73 (13) 47 (17) dizziness 11 (2) 43 (8) 19 (7) headache 11 (2) 26 (5) 9 (3) 6.2 post-marketing experience the following events have been reported during postapproval use of carisoprodol. 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. cardiovascular: tachycardia, postural hypotension, and facial flushing [see overdosage (10) ]. central nervous system: drowsiness, dizziness, vertigo, ataxia, tremor, agitation, irritability, headache, depressive reactions, syncope, insomnia, and seizures [see overdosage (10) ] . gastrointestinal: nausea, vomiting, and epigastric discomfort. hematologic: leukopenia, pancytopenia.

result in decreased exposure of carisoprodol and increased exposure of meprobamate. low dose aspirin also showed an induction effect on cyp2c19. the full pharmacological impact of these potential alterations of exposures in terms of either efficacy or safety of carisoprodol is unknown.

eneral population, the estimated background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2 to 4% and 15 to 20%, respectively. data human data retrospective case-control and cohort studies of meprobamate use during the first trimester of pregnancy have not consistently identified an increased risk or pattern of major birth defects. for children exposed to meprobamate in-utero , one study found no adverse effect on mental or motor development or iq scores. animal data embryofetal development studies in animals have not been completed. in a published pre-and post-natal development animal study, pregnant mice administered carisoprodol orally at 300, 750, or 1200 mg/kg/day (approximately 1-, 2.6-, and 4.1-times the mrhd based on bsa comparison) from 7-days prior to gestation through birth and from lactation through weaning resulted in reduced fetal weights, postnatal weight gain, and postnatal survival at 2.6-and 4.1-times the mrhd. 8.2 lactation risk summary data from published literature report that carisoprodol and its metabolite, meprobamate, are present in breastmilk. there are no data on the effect of carisoprodol on milk production. there is one report of sedation in an infant who was breastfed by a mother taking carisoprodol (see clinical considerations). because there have been no consistent reports of adverse events in breastfed infants over decades of use, the developmental and health benefits of breastfeeding should be considered along with the mother’s clinical need for carisoprodol and any potential adverse effects on the breastfed infant from carisoprodol or from the underlying maternal condition. clinical considerations infants exposed to carisoprodol through breast milk should be monitored for sedation. 8.4 pediatric use the efficacy, safety, and pharmacokinetics of carisoprodol in pediatric patients less than 16 years of age have not been established. 8.5 geriatric use the efficacy, safety, and pharmacokinetics of carisoprodol in patients over 65 years old have not been established. 8.6 renal impairment the safety and pharmacokinetics of carisoprodol in patients with renal impairment have not been evaluated. since carisoprodol is excreted by the kidney, caution should be exercised if carisoprodol is administered to patients with impaired renal function. carisoprodol is dialyzable by hemodialysis and peritoneal dialysis. 8.7 hepatic impairment the safety and pharmacokinetics of carisoprodol in patients with hepatic impairment have not been evaluated. since carisoprodol is metabolized in the liver, caution should be exercised if carisoprodol is administered to patients with impaired hepatic function. 8.8 patients with reduced cyp2c19 activity patients with reduced cyp2c19 activity have higher exposure to carisoprodol. therefore, caution should be exercised in administration of carisoprodol to these patients [see clinical pharmacology (12.3) ] .

ed background risk of major birth defects and miscarriage in clinically recognized pregnancies is 2 to 4% and 15 to 20%, respectively. data human data retrospective case-control and cohort studies of meprobamate use during the first trimester of pregnancy have not consistently identified an increased risk or pattern of major birth defects. for children exposed to meprobamate in-utero , one study found no adverse effect on mental or motor development or iq scores. animal data embryofetal development studies in animals have not been completed. in a published pre-and post-natal development animal study, pregnant mice administered carisoprodol orally at 300, 750, or 1200 mg/kg/day (approximately 1-, 2.6-, and 4.1-times the mrhd based on bsa comparison) from 7-days prior to gestation through birth and from lactation through weaning resulted in reduced fetal weights, postnatal weight gain, and postnatal survival at 2.6-and 4.1-times the mrhd.

rodol and meprobamate was dose proportional between the 250 mg and 350 mg doses. the c max of meprobamate was 2.5 ± 0.5 mcg/ml (mean ± sd) after administration of a single 350 mg dose of carisoprodol, which is approximately 30% of the c max of meprobamate (approximately 8 mcg/ml) after administration of a single 400 mg dose of meprobamate. table 2. pharmacokinetic parameters of carisoprodol and meprobamate (mean ± sd, n=24) 250 mg carisoprodol 350 mg carisoprodol carisoprodol c max (mcg/ml) 1.2 ± 0.5 1.8 ± 1 auc inf (mcg * hr/ml) 4.5 ± 3.1 7 ± 5 t max (hr) 1.5 ± 0.8 1.7 ± 0.8 t 1/2 (hr) 1.7 ± 0.5 2 ± 0.5 meprobamate c max (mcg/ml) 1.8 ± 0.3 2.5 ± 0.5 auc inf (mcg * hr/ml) 32 ± 6.2 46 ± 9 t max (hr) 3.6 ± 1.7 4.5 ± 1.9 t 1/2 (hr) 9.7 ± 1.7 9.6 ± 1.5 absolute bioavailability of carisoprodol has not been determined. the mean time to peak plasma concentrations (t max ) of carisoprodol was approximately 1.5 to 2 hours. food effect: co-administration of a high-fat meal with carisoprodol (350 mg tablet) had no effect on the pharmacokinetics of carisoprodol. therefore, carisoprodol may be administered with or without food. elimination metabolism: the major pathway of carisoprodol metabolism is via the liver by cytochrome enzyme cyp2c19 to form meprobamate. this enzyme exhibits genetic polymorphism (see patients with reduced cyp2c19 activity below). excretion: carisoprodol is eliminated by both renal and non-renal routes with a terminal elimination half-life of approximately 2 hours. the half-life of meprobamate is approximately 10 hours. specific populations sex: exposure of carisoprodol is higher in female than in male subjects (approximately 30 to 50% on a weight adjusted basis). overall exposure of meprobamate is comparable between female and male subjects. patients with reduced cyp2c19 activity: carisoprodol should be used with caution in patients with reduced cyp2c19 activity. published studies indicate that patients who are poor cyp2c19 metabolizers have a 4-fold increase in exposure to carisoprodol, and concomitant 50% reduced exposure to meprobamate compared to normal cyp2c19 metabolizers. the prevalence of poor metabolizers in caucasians and african americans is approximately 3 to 5% and in asians is approximately 15 to 20%.

r) 3.6 ± 1.7 4.5 ± 1.9 t 1/2 (hr) 9.7 ± 1.7 9.6 ± 1.5 absolute bioavailability of carisoprodol has not been determined. the mean time to peak plasma concentrations (t max ) of carisoprodol was approximately 1.5 to 2 hours. food effect: co-administration of a high-fat meal with carisoprodol (350 mg tablet) had no effect on the pharmacokinetics of carisoprodol. therefore, carisoprodol may be administered with or without food. elimination metabolism: the major pathway of carisoprodol metabolism is via the liver by cytochrome enzyme cyp2c19 to form meprobamate. this enzyme exhibits genetic polymorphism (see patients with reduced cyp2c19 activity below). excretion: carisoprodol is eliminated by both renal and non-renal routes with a terminal elimination half-life of approximately 2 hours. the half-life of meprobamate is approximately 10 hours. specific populations sex: exposure of carisoprodol is higher in female than in male subjects (approximately 30 to 50% on a weight adjusted basis). overall exposure of meprobamate is comparable between female and male subjects. patients with reduced cyp2c19 activity: carisoprodol should be used with caution in patients with reduced cyp2c19 activity. published studies indicate that patients who are poor cyp2c19 metabolizers have a 4-fold increase in exposure to carisoprodol, and concomitant 50% reduced exposure to meprobamate compared to normal cyp2c19 metabolizers. the prevalence of poor metabolizers in caucasians and african americans is approximately 3 to 5% and in asians is approximately 15 to 20%.

fertility. a published reproductive study in which female mice received carisoprodol orally at doses of 300, 750, or 1200 mg/kg/day (approximately 1, 2.6, and 4.1 times the mrhd of 1400 mg per day [350 mg qid] based on body surface area [bsa] comparison) from 1-week prior to mating, to 27-weeks post-mating found no alteration in fertility although an alteration in reproductive cycles characterized by a greater time spent in estrus was observed at a carisoprodol dose of 1200 mg/kg/day. in a 13-week toxicology study that did not determine fertility, mouse testes weight and sperm motility were reduced at a dose of 1200 mg/kg/day (maternal doses equivalent to 4.2-times the mrhd based on bsa comparison). in both studies, the no effect level was 750 mg/kg/day, corresponding to approximately 2.6-times the mrhd based on a bsa comparison. the significance of these findings for human fertility is not known.

productive study in which female mice received carisoprodol orally at doses of 300, 750, or 1200 mg/kg/day (approximately 1, 2.6, and 4.1 times the mrhd of 1400 mg per day [350 mg qid] based on body surface area [bsa] comparison) from 1-week prior to mating, to 27-weeks post-mating found no alteration in fertility although an alteration in reproductive cycles characterized by a greater time spent in estrus was observed at a carisoprodol dose of 1200 mg/kg/day. in a 13-week toxicology study that did not determine fertility, mouse testes weight and sperm motility were reduced at a dose of 1200 mg/kg/day (maternal doses equivalent to 4.2-times the mrhd based on bsa comparison). in both studies, the no effect level was 750 mg/kg/day, corresponding to approximately 2.6-times the mrhd based on a bsa comparison. the significance of these findings for human fertility is not known.

(i.e., carisoprodol 250 mg, carisoprodol 350 mg, or placebo) and in study 2 patients were randomized to two treatment groups (i.e., carisoprodol 250 mg or placebo). in both studies, patients received study medication three times a day and at bedtime for seven days. the primary endpoints were the relief from starting backache and the global impression of change, as reported by patients, on study day 3. both endpoints were scored on a 5-point rating scale from 0 (worst outcome) to 4 (best outcome) in both studies. the primary statistical comparison was between the carisoprodol 250 mg and placebo groups in both studies. the proportion of patients who used concomitant acetaminophen, nsaids, tramadol, opioid agonists, other muscle relaxants, and benzodiazepines was similar in the treatment groups. the results for the primary efficacy evaluations in the acute, low back pain studies are presented in table 3. a the primary efficacy endpoints (relief from starting backache and global impression of change) were assessed by the patients on study day 3. these endpoints were scored on a 5-point rating scale from 0 (worst outcome) to 4 (best outcome). b mean is the least squared mean and se is the standard error of the mean. the anova model was used for the primary statistical comparison between the carisoprodol 250 mg and placebo groups. table 3. results of the primary efficacy endpoints a in studies 1 and 2 study parameter placebo carisoprodol 250 mg carisoprodol 350 mg 1 number of patients n=269 n=264 n=273 relief from starting backache, mean (se) b 1.4 (0.1) 1.8 (0.1) 1.8 (0.1) difference between carisoprodol and placebo, mean (se) b (95% ci) 0.4 (0.2, 0.5) 0.4 (0.2, 0.6) global impression of change, mean (se) b 1.9 (0.1) 2.2 (0.1) 2.2 (0.1) difference between carisoprodol and placebo, mean (se) b (95% ci) 0.2 (0.1, 0.4) 0.3 (0.1, 0.4) 2 number of patients n=278 n=269 relief from starting backache, mean (se) b 1.1 (0.1) 1.8 (0.1) difference between carisoprodol and placebo, mean (se) b (95% ci) 0.7 (0.5, 0.9) global impression of change, mean (se) b 1.7 (0.1) 2.2 (0.1) difference between carisoprodol and placebo, mean (se) b (95% ci) 0.5 (0.4, 0.7) patients treated with carisoprodol experienced improvement in function as measured by the roland-morris disability questionnaire (rmdq) score on days 3 and 7.

e, musculoskeletal discomfort. in the post-marketing experience with carisoprodol, cases of dependence, withdrawal, and abuse have been reported with prolonged use. if the musculoskeletal symptoms still persist, patients should contact their healthcare provider for further evaluation. lactation advise nursing mothers using carisoprodol to monitor neonates for signs of sedation [see use in specific populations (8.2) ]. distributed by: aurobindo pharma usa, inc. 279 princeton-hightstown road east windsor, nj 08520 manufactured by: aurobindo pharma limited hyderabad-500 032, india revised: 11/2021