WebSite Houston

Monday, November 14, 2016

Carbamazepine

Carbamazepine TABLETS USP, 200 mg/Carbamazepine TABLETS, USP (CHEWABLE), 100 mg

0109

0778

Rx only

Prescribing Information

WARNINGS

SERIOUS DERMATOLOGIC REACTIONS AND HLA-B*1502 ALLELE

SERIOUS AND SOMETIMES FATAL DERMATOLOGIC REACTIONS, INCLUDING TOXIC EPIDERMAL NECROLYSIS (TEN) AND STEVENS-JOHNSON SYNDROME (SJS), HAVE BEEN REPORTED DURING TREATMENT WITH Carbamazepine. THESE REACTIONS ARE ESTIMATED TO OCCUR IN 1 TO 6 PER 10,000 NEW USERS IN COUNTRIES WITH MAINLY CAUCASIAN POPULATIONS, BUT THE RISK IN SOME ASIAN COUNTRIES IS ESTIMATED TO BE ABOUT 10 TIMES HIGHER. STUDIES IN PATIENTS OF CHINESE ANCESTRY HAVE FOUND A STRONG ASSOCIATION BETWEEN THE RISK OF DEVELOPING SJS/TEN AND THE PRESENCE OF HLA-B*1502, AN INHERITED ALLELIC VARIANT OF THE HLA-B GENE. HLA-B*1502 IS FOUND ALMOST EXCLUSIVELY IN PATIENTS WITH ANCESTRY ACROSS BROAD AREAS OF ASIA. PATIENTS WITH ANCESTRY IN GENETICALLY AT-RISK POPULATIONS SHOULD BE SCREENED FOR THE PRESENCE OF HLA-B*1502 PRIOR TO INITIATING TREATMENT WITH Carbamazepine. PATIENTS TESTING POSITIVE FOR THE ALLELE SHOULD NOT BE TREATED WITH Carbamazepine UNLESS THE BENEFIT CLEARLY OUTWEIGHS THE RISK (SEE WARNINGS AND PRECAUTIONS, Laboratory Tests).

APLASTIC ANEMIA AND AGRANULOCYTOSIS

APLASTIC ANEMIA AND AGRANULOCYTOSIS HAVE BEEN REPORTED IN ASSOCIATION WITH THE USE OF Carbamazepine. DATA FROM A POPULATION-BASED CASE CONTROL STUDY DEMONSTRATE THAT THE RISK OF DEVELOPING THESE REACTIONS IS 5 TO 8 TIMES GREATER THAN IN THE GENERAL POPULATION. HOWEVER, THE OVERALL RISK OF THESE REACTIONS IN THE UNTREATED GENERAL POPULATION IS LOW, APPROXIMATELY SIX PATIENTS PER ONE MILLION POPULATION PER YEAR FOR AGRANULOCYTOSIS AND TWO PATIENTS PER ONE MILLION POPULATION PER YEAR FOR APLASTIC ANEMIA.

ALTHOUGH REPORTS OF TRANSIENT OR PERSISTENT DECREASED PLATELET OR WHITE BLOOD CELL COUNTS ARE NOT UNCOMMON IN ASSOCIATION WITH THE USE OF Carbamazepine, DATA ARE NOT AVAILABLE TO ESTIMATE ACCURATELY THEIR INCIDENCE OR OUTCOME. HOWEVER, THE VAST MAJORITY OF THE CASES OF LEUKOPENIA HAVE NOT PROGRESSED TO THE MORE SERIOUS CONDITIONS OF APLASTIC ANEMIA OR AGRANULOCYTOSIS.

BECAUSE OF THE VERY LOW INCIDENCE OF AGRANULOCYTOSIS AND APLASTIC ANEMIA, THE VAST MAJORITY OF MINOR HEMATOLOGIC CHANGES OBSERVED IN MONITORING OF PATIENTS ON Carbamazepine ARE UNLIKELY TO SIGNAL THE OCCURRENCE OF EITHER ABNORMALITY. NONETHELESS, COMPLETE PRETREATMENT HEMATOLOGICAL TESTING SHOULD BE OBTAINED AS A BASELINE. IF A PATIENT IN THE COURSE OF TREATMENT EXHIBITS LOW OR DECREASED WHITE BLOOD CELL OR PLATELET COUNTS, THE PATIENT SHOULD BE MONITORED CLOSELY. DISCONTINUATION OF THE DRUG SHOULD BE CONSIDERED IF ANY EVIDENCE OF SIGNIFICANT BONE MARROW DEPRESSION DEVELOPS.

Before prescribing Carbamazepine, the physician should be thoroughly familiar with the details of this prescribing information, particularly regarding use with other drugs, especially those which accentuate toxicity potential.

Carbamazepine Description

Carbamazepine USP is an anticonvulsant and specific analgesic for trigeminal neuralgia, available for oral administration as chewable tablets of 100 mg and tablets of 200 mg. Its chemical name is 5H-dibenz[b,f]azepine-5-carboxamide, and its structural formula is:

C15H12N2O M.W. 236.27

Carbamazepine USP is a white to off-white powder, practically insoluble in water and soluble in alcohol and in acetone.

Carbamazepine tablets USP, 200 mg contain the inactive ingredients colloidal silicon dioxide, croscarmellose sodium, ethylcellulose, glycerin, lactose monohydrate, magnesium stearate, and sodium starch glycolate.

Carbamazepine tablets, USP (chewable), 100 mg contain the inactive ingredients acacia, colloidal silicon dioxide, croscarmellose sodium, ethylcellulose, FD&C Red #40 aluminum lake, flavoring, glycerin, lactose monohydrate, magnesium stearate, pregelatinized corn starch, and sucrose.

Carbamazepine tablets USP, 200 mg meet USP Dissolution Test 3.

Carbamazepine tablets, USP (chewable), 100 mg meet USP Dissolution Test 1.

Carbamazepine - Clinical Pharmacology

In controlled clinical trials, Carbamazepine has been shown to be effective in the treatment of psychomotor and grand mal seizures, as well as trigeminal neuralgia.

Mechanism of Action

Carbamazepine has demonstrated anticonvulsant properties in rats and mice with electrically and chemically induced seizures. It appears to act by reducing polysynaptic responses and blocking the post-tetanic potentiation. Carbamazepine greatly reduces or abolishes pain induced by stimulation of the infraorbital nerve in cats and rats. It depresses thalamic potential and bulbar and polysynaptic reflexes, including the linguomandibular reflex in cats. Carbamazepine is chemically unrelated to other anticonvulsants or other drugs used to control the pain of trigeminal neuralgia. The mechanism of action remains unknown.

The principal metabolite of Carbamazepine, Carbamazepine-10,11-epoxide, has anticonvulsant activity as demonstrated in several in vivo animal models of seizures. Though clinical activity for the epoxide has been postulated, the significance of its activity with respect to the safety and efficacy of Carbamazepine has not been established.

Pharmacokinetics

In clinical studies, Carbamazepine suspension, conventional tablets, and extended-release tablets delivered equivalent amounts of drug to the systemic circulation. However, the suspension was absorbed somewhat faster, and the extended-release tablet slightly slower, than the conventional tablet. The bioavailability of the extended-release tablet was 89% compared to suspension. Following a b.i.d. dosage regimen, the suspension provides higher peak levels and lower trough levels than those obtained from the conventional tablet for the same dosage regimen. On the other hand, following a t.i.d. dosage regimen, Carbamazepine suspension affords steady-state plasma levels comparable to Carbamazepine tablets given b.i.d. when administered at the same total mg daily dose. Following a b.i.d. dosage regimen, Carbamazepine extended-release tablets afford steady-state plasma levels comparable to conventional Carbamazepine tablets given q.i.d., when administered at the same total mg daily dose. Carbamazepine in blood is 76% bound to plasma proteins. Plasma levels of Carbamazepine are variable and may range from 0.5 to 25 mcg/mL, with no apparent relationship to the daily intake of the drug. Usual adult therapeutic levels are between 4 and 12 mcg/mL. In polytherapy, the concentration of Carbamazepine and concomitant drugs may be increased or decreased during therapy, and drug effects may be altered (see PRECAUTIONS, Drug Interactions). Following chronic oral administration of suspension, plasma levels peak at approximately 1.5 hours compared to 4 to 5 hours after administration of conventional Carbamazepine tablets, and 3 to 12 hours after administration of Carbamazepine extended-release tablets. The CSF/serum ratio is 0.22, similar to the 24% unbound Carbamazepine in serum. Because Carbamazepine induces its own metabolism, the half-life is also variable. Autoinduction is completed after 3 to 5 weeks of a fixed dosing regimen. Initial half-life values range from 25 to 65 hours, decreasing to 12 to 17 hours on repeated doses. Carbamazepine is metabolized in the liver. Cytochrome P450 3A4 was identified as the major isoform responsible for the formation of Carbamazepine-10,11-epoxide from Carbamazepine. After oral administration of 14C-Carbamazepine, 72% of the administered radioactivity was found in the urine and 28% in the feces. This urinary radioactivity was composed largely of hydroxylated and conjugated metabolites, with only 3% of unchanged Carbamazepine.

The pharmacokinetic parameters of Carbamazepine disposition are similar in children and in adults. However, there is a poor correlation between plasma concentrations of Carbamazepine and Carbamazepine dose in children. Carbamazepine is more rapidly metabolized to Carbamazepine-10,11-epoxide (a metabolite shown to be equipotent to Carbamazepine as an anticonvulsant in animal screens) in the younger age groups than in adults. In children below the age of 15, there is an inverse relationship between CBZ-E/CBZ ratio and increasing age (in one report from 0.44 in children below the age of 1 year to 0.18 in children between 10 to 15 years of age).

The effects of race and gender on Carbamazepine pharmacokinetics have not been systematically evaluated.

Indications and Usage for Carbamazepine

Epilepsy

Carbamazepine is indicated for use as an anticonvulsant drug. Evidence supporting efficacy of Carbamazepine as an anticonvulsant was derived from active drug-controlled studies that enrolled patients with the following seizure types:

Partial seizures with complex symptomatology (psychomotor, temporal lobe). Patients with these seizures appear to show greater improvement than those with other types.

Generalized tonic-clonic seizures (grand mal).

Mixed seizure patterns which include the above, or other partial or generalized seizures. Absence seizures (petit mal) do not appear to be controlled by Carbamazepine (see PRECAUTIONS, General).

Trigeminal Neuralgia

Carbamazepine is indicated in the treatment of the pain associated with true trigeminal neuralgia.

Beneficial results have also been reported in glossopharyngeal neuralgia.

This drug is not a simple analgesic and should not be used for the relief of trivial aches or pains.

Contraindications

Carbamazepine should not be used in patients with a history of previous bone marrow depression, hypersensitivity to the drug, or known sensitivity to any of the tricyclic compounds, such as amitriptyline, desipramine, imipramine, protriptyline, nortriptyline, etc. Likewise, on theoretical grounds its use with monoamine oxidase inhibitors is not recommended. Before administration of Carbamazepine, MAO inhibitors should be discontinued for a minimum of 14 days, or longer if the clinical situation permits.

Coadministration of Carbamazepine and nefazodone may result in insufficient plasma concentrations of nefazodone and its active metabolite to achieve a therapeutic effect. Coadministration of Carbamazepine with nefazodone is contraindicated.

Warnings

Serious Dermatologic Reactions

Serious and sometimes fatal dermatologic reactions, including toxic epidermal necrolysis (TEN) and Stevens-Johnson syndrome (SJS), have been reported with Carbamazepine treatment. The risk of these events is estimated to be about 1 to 6 per 10,000 new users in countries with mainly Caucasian populations. However, the risk in some Asian countries is estimated to be about 10 times higher. Carbamazepine should be discontinued at the first sign of a rash, unless the rash is clearly not drug-related. If signs or symptoms suggest SJS/TEN, use of this drug should not be resumed and alternative therapy should be considered.

SJS/TEN and HLA-B*1502 Allele

Retrospective case-control studies have found that in patients of Chinese ancestry there is a strong association between the risk of developing SJS/TEN with Carbamazepine treatment and the presence of an inherited variant of the HLA-B gene, HLA-B*1502. The occurrence of higher rates of these reactions in countries with higher frequencies of this allele suggests that the risk may be increased in allele-positive individuals of any ethnicity.

Across Asian populations, notable variation exists in the prevalence of HLA-B*1502. Greater than 15% of the population is reported positive in Hong Kong, Thailand, Malaysia, and parts of the Philippines, compared to about 10% in Taiwan and 4% in North China. South Asians, including Indians, appear to have intermediate prevalence of HLA-B*1502, averaging 2 to 4%, but higher in some groups. HLA-B*1502 is present in < 1% of the population in Japan and Korea.

HLA-B*1502 is largely absent in individuals not of Asian origin (e.g., Caucasians, African-Americans, Hispanics, and Native Americans).

Prior to initiating Carbamazepine therapy, testing for HLA-B*1502 should be performed in patients with ancestry in populations in which HLA-B*1502 may be present. In deciding which patients to screen, the rates provided above for the prevalence of HLA-B*1502 may offer a rough guide, keeping in mind the limitations of these figures due to wide variability in rates even within ethnic groups, the difficulty in ascertaining ethnic ancestry, and the likelihood of mixed ancestry. Carbamazepine should not be used in patients positive for HLA-B*1502 unless the benefits clearly outweigh the risks. Tested patients who are found to be negative for the allele are thought to have a low risk of SJS/TEN (see WARNINGS and PRECAUTIONS, Laboratory Tests).

Over 90% of Carbamazepine treated patients who will experience SJS/TEN have this reaction within the first few months of treatment. This information may be taken into consideration in determining the need for screening of genetically at-risk patients currently on Carbamazepine.

The HLA-B*1502 allele has not been found to predict risk of less severe adverse cutaneous reactions from Carbamazepine, such as anticonvulsant hypersensitivity syndrome or nonserious rash (maculopapular eruption [MPE]).

Limited evidence suggests that HLA-B*1502 may be a risk factor for the development of SJS/TEN in patients of Chinese ancestry taking other antiepileptic drugs associated with SJS/TEN. Consideration should be given to avoiding use of other drugs associated with SJS/TEN in HLA-B*1502 positive patients, when alternative therapies are otherwise equally acceptable.

Application of HLA-B*1502 genotyping as a screening tool has important limitations and must never substitute for appropriate clinical vigilance and patient management. Many HLA-B*1502-positive Asian patients treated with Carbamazepine will not develop SJS/TEN, and these reactions can still occur infrequently in HLA-B*1502-negative patients of any ethnicity. The role of other possible factors in the development of, and morbidity from, SJS/TEN, such as antiepileptic drug (AED) dose, compliance, concomitant medications, comorbidities, and the level of dermatologic monitoring have not been studied.

Aplastic Anemia and Agranulocytosis

Patients with a history of adverse hematologic reaction to any drug may be particularly at risk of bone marrow depression.

Suicidal Behavior and Ideation

Antiepileptic drugs (AEDs), including Carbamazepine, increase the risk of suicidal thoughts or behavior in patients taking these drugs for any indication. Patients treated with any AED for any indication should be monitored for the emergence or worsening of depression, suicidal thoughts or behavior, and/or any unusual changes in mood or behavior.

Pooled analyses of 199 placebo-controlled clinical trials (mono- and adjunctive therapy) of 11 different AEDs showed that patients randomized to one of the AEDs had approximately twice the risk (adjusted Relative Risk 1.8, 95% CI:1.2, 2.7) of suicidal thinking or behavior compared to patients randomized to placebo. In these trials, which had a median treatment duration of 12 weeks, the estimated incidence rate of suicidal behavior or ideation among 27,863 AED-treated patients was 0.43%, compared to 0.24% among 16,029 placebo-treated patients, representing an increase of approximately one case of suicidal thinking or behavior for every 530 patients treated. There were four suicides in drug-treated patients in the trials and none in placebo-treated patients, but the number is too small to allow any conclusion about drug effect on suicide.

The increased risk of suicidal thoughts or behavior with AEDs was observed as early as one week after starting drug treatment with AEDs and persisted for the duration of treatment assessed. Because most trials included in the analysis did not extend beyond 24 weeks, the risk of suicidal thoughts or behavior beyond 24 weeks could not be assessed.

The risk of suicidal thoughts or behavior was generally consistent among drugs in the data analyzed. The finding of increased risk with AEDs of varying mechanisms of action and across a range of indications suggests that the risk applies to all AEDs used for any indication. The risk did not vary substantially by age (5 to 100 years) in the clinical trials analyzed. Table 1 shows absolute and relative risk by indication for all evaluated AEDs.

Table 1: Risk by Indication for Antiepileptic Drugs in the Pooled Analysis
Indication	Placebo Patients with Events Per 1,000 Patients	Drug Patients with Events Per 1,000 Patients	Relative Risk: Incidence of Events in Drug Patients/Incidence in Placebo Patients	Risk Difference: Additional Drug Patients with Events Per 1,000 Patients
Epilepsy	1.0	3.4	3.5	2.4
Psychiatric	5.7	8.5	1.5	2.9
Other	1.0	1.8	1.9	0.9
Total	2.4	4.3	1.8	1.9

The relative risk for suicidal thoughts or behavior was higher in clinical trials for epilepsy than in clinical trials for psychiatric or other conditions, but the absolute risk differences were similar for the epilepsy and psychiatric indications.

Anyone considering prescribing Carbamazepine or any other AED must balance the risk of suicidal thoughts or behavior with the risk of untreated illness. Epilepsy and many other illnesses for which AEDs are prescribed are themselves associated with morbidity and mortality and an increased risk of suicidal thoughts and behavior. Should suicidal thoughts and behavior emerge during treatment, the prescriber needs to consider whether the emergence of these symptoms in any given patient may be related to the illness being treated.

Patients, their caregivers, and families should be informed that AEDs increase the risk of suicidal thoughts and behavior and should be advised of the need to be alert for the emergence or worsening of the signs and symptoms of depression, any unusual changes in mood or behavior, or the emergence of suicidal thoughts, behavior, or thoughts about self-harm. Behaviors of concern should be reported immediately to healthcare providers.

General

Carbamazepine has shown mild anticholinergic activity; therefore, patients with increased intraocular pressure should be closely observed during therapy.

Because of the relationship of the drug to other tricyclic compounds, the possibility of activation of a latent psychosis and, in elderly patients, of confusion or agitation should be borne in mind.

The use of Carbamazepine should be avoided in patients with a history of hepatic porphyria (e.g., acute intermittent porphyria, variegate porphyria, porphyria cutanea tarda). Acute attacks have been reported in such patients receiving Carbamazepine therapy. Carbamazepine administration has also been demonstrated to increase porphyrin precursors in rodents, a presumed mechanism for the induction of acute attacks of porphyria.

As with all antiepileptic drugs, Carbamazepine should be withdrawn gradually to minimize the potential of increased seizure frequency.

Usage in Pregnancy

Carbamazepine can cause fetal harm when administered to a pregnant woman.

Epidemiological data suggest that there may be an association between the use of Carbamazepine during pregnancy and congenital malformations, including spina bifida. There have also been reports that associate Carbamazepine with developmental disorders and congenital anomalies (e.g., craniofacial defects, cardiovascular malformations, hypospadias and anomalies involving various body systems). Developmental delays based on neurobehavioral assessments have been reported. In treating or counseling women of childbearing potential, the prescribing physician will wish to weigh the benefits of therapy against the risks. If this drug is used during pregnancy, or if the patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus.

Retrospective case reviews suggest that, compared with monotherapy, there may be a higher prevalence of teratogenic effects associated with the use of anticonvulsants in combination therapy. Therefore, if therapy is to be continued, monotherapy may be preferable for pregnant women.

In humans, transplacental passage of Carbamazepine is rapid (30 to 60 minutes), and the drug is accumulated in the fetal tissues, with higher levels found in liver and kidney than in brain and lung.

Carbamazepine has been shown to have adverse effects in reproduction studies in rats when given orally in dosages 10 to 25 times the maximum human daily dosage (MHDD) of 1200 mg on a mg/kg basis or 1.5 to 4 times the MHDD on a mg/m2 basis. In rat teratology studies, 2 of 135 offspring showed kinked ribs at 250 mg/kg and 4 of 119 offspring at 650 mg/kg showed other anomalies (cleft palate, 1; talipes, 1; anophthalmos, 2). In reproduction studies in rats, nursing offspring demonstrated a lack of weight gain and an unkempt appearance at a maternal dosage level of 200 mg/kg.

Antiepileptic drugs should not be discontinued abruptly in patients in whom the drug is administered to prevent major seizures because of the strong possibility of precipitating status epilepticus with attendant hypoxia and threat to life. In individual cases where the severity and frequency of the seizure disorder are such that removal of medication does not pose a serious threat to the patient, discontinuation of the drug may be considered prior to and during pregnancy, although it cannot be said with any confidence that even minor seizures do not pose some hazard to the developing embryo or fetus.

Tests to detect defects using currently accepted procedures should be considered a part of routine prenatal care in childbearing women receiving Carbamazepine.

There have been a few cases of neonatal seizures and/or respiratory depression associated with maternal Carbamazepine and other concomitant anticonvulsant drug use. A few cases of neonatal vomiting, diarrhea, and/or decreased feeding have also been reported in association with maternal Carbamazepine use. These symptoms may represent a neonatal withdrawal syndrome.

To provide information regarding the effects of in utero exposure to Carbamazepine, physicians are advised to recommend that pregnant patients taking Carbamazepine enroll in the North American Antiepileptic Drug (NAAED) Pregnancy Registry. This can be done by calling the toll free number 1-888-233-2334, and must be done by patients themselves. Information on the registry can also be found at the website http://www.aedpregnancyregistry.org/.

Precautions

General

Before initiating therapy, a detailed history and physical examination should be made.

Carbamazepine should be used with caution in patients with a mixed seizure disorder that includes atypical absence seizures, since in these patients Carbamazepine has been associated with increased frequency of generalized convulsions (see INDICATIONS AND USAGE).

Therapy should be prescribed only after critical benefit-to-risk appraisal in patients with a history of cardiac conduction disturbance, including second and third degree AV heart block; cardiac, hepatic, or renal damage; adverse hematologic or hypersensitivity reaction to other drugs, including reactions to other anticonvulsants; or interrupted courses of therapy with Carbamazepine.

AV heart block, including second and third degree block, have been reported following Carbamazepine treatment. This occurred generally, but not solely, in patients with underlying EKG abnormalities or risk factors for conduction disturbances.

Hepatic effects, ranging from slight elevations in liver enzymes to rare cases of hepatic failure have been reported (see ADVERSE REACTIONS and PRECAUTIONS, LaboratoryTests). In some cases, hepatic effects may progress despite discontinuation of the drug.

Multiorgan hypersensitivity reactions which can affect the skin, liver, hemopoietic organs and lymphatic system or other organs and occurring days to weeks or months after initiating treatment have been reported in rare cases (see ADVERSE REACTIONS, Other and PRECAUTIONS, Information for Patients).

Discontinuation of Carbamazepine should be considered if any evidence of hypersensitivity develops.

Hypersensitivity reactions to Carbamazepine have been reported in patients who previously experienced this reaction to anticonvulsants including phenytoin and phenobarbital. A history of hypersensitivity reactions should be obtained for a patient and the immediate family members. If positive, caution should be used in prescribing Carbamazepine.

In patients who have exhibited hypersensitivity reactions to Carbamazepine approximately 25 to 30% of these patients may experience hypersensitivity reactions with oxcarbazepine.

Information for Patients

Patients should be informed of the availability of a Medication Guide and they should be instructed to read the Medication Guide before taking Carbamazepine.

Patients should be made aware of the early toxic signs and symptoms of a potential hematologic problem, as well as dermatologic, hypersensitivity or hepatic reactions. These symptoms may include, but are not limited to, fever, sore throat, rash, ulcers in the mouth, easy bruising, lymphadenopathy and petechial or purpuric hemorrhage, and in the case of liver reactions, anorexia, nausea/vomiting, or jaundice. The patient should be advised that, because these signs and symptoms may signal a serious reaction, that they must report any occurrence immediately to a physician. In addition, the patient should be advised that these signs and symptoms should be reported even if mild or when occurring after extended use.

Patients, their caregivers, and families should be counseled that AEDs, including Carbamazepine, may increase the risk of suicidal thoughts and behavior and should be advised of the need to be alert for the emergence or worsening of symptoms of depression, any unusual changes in mood or behavior, or the emergence of suicidal thoughts, behavior, or thoughts about self-harm. Behaviors of concern should be reported immediately to healthcare providers.

Patients should be advised that serious skin reactions have been reported in association with Carbamazepine. In the event a skin reaction should occur while taking Carbamazepine, patients should consult with their physician immediately (see WARNINGS).

Carbamazepine may interact with some drugs. Therefore, patients should be advised to report to their doctors the use of any other prescription or nonprescription medications or herbal products.

Caution should be exercised if alcohol is taken in combination with Carbamazepine therapy, due to a possible additive sedative effect.

Since dizziness and drowsiness may occur, patients should be cautioned about the hazards of operating machinery or automobiles or engaging in other potentially dangerous tasks.

Patients should be encouraged to enroll in the NAAED Pregnancy Registry if they become pregnant. This registry is collecting information about the safety of antiepileptic drugs during pregnancy. To enroll, patients can call the toll free number 1-888-233-2334 (see WARNINGS, Usage in Pregnancy).

Laboratory Tests

For genetically at-risk patients (see WARNINGS), high-resolution ‘HLA-B*1502 typing’ is recommended. The test is positive if either one or two HLA-B*1502 alleles are detected and negative if no HLA-B*1502 alleles are detected.

Complete pretreatment blood counts, including platelets and possibly reticulocytes and serum iron, should be obtained as a baseline. If a patient in the course of treatment exhibits low or decreased white blood cell or platelet counts, the patient should be monitored closely. Discontinuation of the drug should be considered if any evidence of significant bone marrow depression develops.

Baseline and periodic evaluations of liver function, particularly in patients with a history of liver disease, must be performed during treatment with this drug since liver damage may occur (see PRECAUTIONS, General and ADVERSE REACTIONS). Carbamazepine should be discontinued, based on clinical judgment, if indicated by newly occurring or worsening clinical or laboratory evidence of liver dysfunction or hepatic damage, or in the case of active liver disease.

Baseline and periodic eye examinations, including slit-lamp, funduscopy, and tonometry, are recommended since many phenothiazines and related drugs have been shown to cause eye changes.

Baseline and periodic complete urinalysis and BUN determinations are recommended for patients treated with this agent because of observed renal dysfunction.

Monitoring of blood levels (see CLINICAL PHARMACOLOGY) has increased the efficacy and safety of anticonvulsants. This monitoring may be particularly useful in cases of dramatic increase in seizure frequency and for verification of compliance. In addition, measurement of drug serum levels may aid in determining the cause of toxicity when more than one medication is being used.

Thyroid function tests have been reported to show decreased values with Carbamazepine administered alone.

Hyponatremia has been reported in association with Carbamazepine use, either alone or in combination with other drugs.

Interference with some pregnancy tests has been reported.

Drug Interactions

Clinically meaningful drug interactions have occurred with concomitant medications and include, but are not limited to, the following:

Agents That May Affect Carbamazepine Plasma Levels

CYP 3A4 inhibitors inhibit Carbamazepine metabolism and can thus increase plasma Carbamazepine levels. Drugs that have been shown, or would be expected, to increase plasma Carbamazepine levels include:

cimetidine, danazol, diltiazem, macrolides, erythromycin, troleandomycin, clarithromycin, fluoxetine, fluvoxamine, nefazodone, trazodone, loxapine*, olanzapine, quetiapine*, loratadine, terfenadine, omeprazole, oxybutynin, dantrolene, isoniazid, niacinamide, nicotinamide, ibuprofen, propoxyphene, azoles (e.g., ketoconazole, itraconazole, fluconazole, voriconazole), acetazolamide, verapamil, ticlopidine, grapefruit juice, protease inhibitors, valproate*.

CYP 3A4 inducers can increase the rate of Carbamazepine metabolism. Drugs that have been shown, or that would be expected, to decrease plasma Carbamazepine levels include:

cisplatin, doxorubicin HCl, felbamate†, fosphenytoin, rifampin, phenobarbital, phenytoin, primidone, methsuximide, theophylline, aminophylline.

When Carbamazepine is given with drugs that can increase or decrease Carbamazepine levels, close monitoring of Carbamazepine levels is indicated and dosage adjustment may be required.

* increased levels of the active 10,11-epoxide

† decreased levels of Carbamazepine and increased levels of the 10,11-epoxide

Effect of Carbamazepine on Plasma Levels of Concomitant Agents

Increased levels: clomipramine HCl, phenytoin, primidone

Carbamazepine is a potent inducer of hepatic CYP 3A4 and may therefore reduce plasma concentrations of comedications mainly metabolized by 3A4 through induction of their metabolism. Carbamazepine causes, or would be expected to cause, decreased levels of the following:

acetaminophen, alprazolam, bupropion, dihydropyridine calcium channel blockers (e.g., felodipine), citalopram, cyclosporine, corticosteroids (e.g., prednisolone, dexamethasone), clonazepam, clozapine, dicumarol, doxycycline, ethosuximide, everolimus, haloperidol, imatinib, itraconazole, lamotrigine, levothyroxine, methadone, methsuximide, midazolam, olanzapine, oral and other hormonal contraceptives, oxcarbazepine, phensuximide, phenytoin, praziquantel, protease inhibitors, risperidone, theophylline, tiagabine, topiramate, tramadol, trazodone, tricyclic antidepressants (e.g., imipramine, amitriptyline, nortriptyline), valproate, warfarin, ziprasidone, zonisamide.

In concomitant use with Carbamazepine, dosage adjustment of the above agents may be necessary.

Coadministration of Carbamazepine with nefazodone results in insufficient plasma concentrations of nefazodone and its active metabolite to achieve a therapeutic effect. Coadministration of Carbamazepine with nefazodone is contraindicated (see CONTRAINDICATIONS).

Concomitant administration of Carbamazepine and lithium may increase the risk of neurotoxic side effects.

Concomitant use of Carbamazepine and isoniazid has been reported to increase isoniazid-induced hepatotoxicity.

Concomitant medication with Carbamazepine and some diuretics (hydrochlorothiazide, furosemide) may lead to symptomatic hyponatremia.

Carbamazepine may antagonize the effects of nondepolarizing muscle relaxants (e.g., pancuronium).

Their dosage may need to be raised, and patients should be monitored closely for more rapid recovery from neuromuscular blockade than expected.

Alterations of thyroid function have been reported in combination therapy with other anticonvulsant medications.

Concomitant use of Carbamazepine with hormonal contraceptive products (e.g., oral, and levonorgestrel subdermal implant contraceptives) may render the contraceptives less effective because the plasma concentrations of the hormones may be decreased. Breakthrough bleeding and unintended pregnancies have been reported. Alternative or back-up methods of contraception should be considered.

Carcinogenesis, Mutagenesis, Impairment of Fertility

Carbamazepine, when administered to Sprague-Dawley rats for two years in the diet at doses of 25, 75, and 250 mg/kg/day, resulted in a dose-related increase in the incidence of hepatocellular tumors in females and of benign interstitial cell adenomas in the testes of males.

Carbamazepine must, therefore, be considered to be carcinogenic in Sprague-Dawley rats. Bacterial and mammalian mutagenicity studies using Carbamazepine produced negative results. The significance of these findings relative to the use of Carbamazepine in humans is, at present, unknown.

Usage in Pregnancy

Teratogenic Effects

Pregnancy category D

(See WARNINGS.)

Labor and Delivery

The effect of Carbamazepine on human labor and delivery is unknown.

Nursing Mothers

Carbamazepine and its epoxide metabolite are transferred to breast milk. The ratio of the concentration in breast milk to that in maternal plasma is about 0.4 for Carbamazepine and about 0.5 for the epoxide. The estimated doses given to the newborn during breast-feeding are in the range of 2 to 5 mg daily for Carbamazepine and 1 to 2 mg daily for the epoxide.

Because of the potential for serious adverse reactions in nursing infants from Carbamazepine, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.

Pediatric Use

Substantial evidence of Carbamazepine’s effectiveness for use in the management of children with epilepsy (see INDICATIONS AND USAGE for specific seizure types) is derived from clinical investigations performed in adults and from studies in several in vitro systems which support the conclusion that (1) the pathogenetic mechanisms underlying seizure propagation are essentially identical in adults and children, and (2) the mechanism of action of Carbamazepine in treating seizures is essentially identical in adults and children.

Taken as a whole, this information supports a conclusion that the generally accepted therapeutic range of total Carbamazepine in plasma (i.e., 4 to 12 mcg/mL) is the same in children and adults.

The evidence assembled was primarily obtained from short-term use of Carbamazepine. The safety of Carbamazepine in children has been systematically studied up to 6 months. No longer-term data from clinical trials is available.

Geriatric Use

No systematic studies in geriatric patients have been conducted.

Adverse Reactions

If adverse reactions are of such severity that the drug must be discontinued, the physician must be aware that abrupt discontinuation of any anticonvulsant drug in a responsive epileptic patient may lead to seizures or even status epilepticus with its life-threatening hazards.

The most severe adverse reactions have been observed in the hemopoietic system and skin (see BOXEDWARNING), the liver, and the cardiovascular system.

The most frequently observed adverse reactions, particularly during the initial phases of therapy, are dizziness, drowsiness, unsteadiness, nausea, and vomiting. To minimize the possibility of such reactions, therapy should be initiated at the low dosage recommended.

The following additional adverse reactions have been reported:

Hemopoietic System: Aplastic anemia, agranulocytosis, pancytopenia, bone marrow depression, thrombocytopenia, leukopenia, leukocytosis, eosinophilia, anemia, acute intermittent porphyria, variegate porphyria, porphyria cutanea tarda.

Skin: Toxic epidermal necrolysis (TEN) and Stevens-Johnson syndrome (SJS) (see BOXEDWARNING), pruritic and erythematous rashes, urticaria, photosensitivity reactions, alterations in skin pigmentation, exfoliative dermatitis, erythema multiforme and nodosum, purpura, aggravation of disseminated lupus erythematosus, alopecia, and diaphoresis. In certain cases, discontinuation of therapy may be necessary. Isolated cases of hirsutism have been reported, but a causal relationship is not clear.

Cardiovascular System: Congestive heart failure, edema, aggravation of hypertension, hypotension, syncope and collapse, aggravation of coronary artery disease, arrhythmias and AV block, thrombophlebitis, thromboembolism (e.g., pulmonary embolism), and adenopathy or lymphadenopathy.

Some of these cardiovascular complications have resulted in fatalities. Myocardial infarction has been associated with other tricyclic compounds.

Liver: Abnormalities in liver function tests, cholestatic and hepatocellular jaundice, hepatitis; very rare cases of hepatic failure.

Pancreatic: Pancreatitis.

Respiratory System: Pulmonary hypersensitivity characterized by fever, dyspnea, pneumonitis, or pneumonia.

Genitourinary System: Urinary frequency, acute urinary retention, oliguria with elevated blood pressure, azotemia, renal failure, and impotence. Albuminuria, glycosuria, elevated BUN, and microscopic deposits in the urine have also been reported. There have been very rare reports of impaired male fertility and/or abnormal spermatogenesis.

Testicular atrophy occurred in rats receiving Carbamazepine orally from 4 to 52 weeks at dosage levels of 50 to 400 mg/kg/day. Additionally, rats receiving Carbamazepine in the diet for 2 years at dosage levels of 25, 75, and 250 mg/kg/day had a dose-related incidence of testicular atrophy and aspermatogenesis. In dogs, it produced a brownish discoloration, presumably a metabolite, in the urinary bladder at dosage levels of 50 mg/kg and higher. Relevance of these findings to humans is unknown.

Nervous System: Dizziness, drowsiness, disturbances of coordination, confusion, headache, fatigue, blurred vision, visual hallucinations, transient diplopia, oculomotor disturbances, nystagmus, speech disturbances, abnormal involuntary movements, peripheral neuritis and paresthesias, depression with agitation, talkativeness, tinnitus, hyperacusis, neuroleptic malignant syndrome.

There have been reports of associated paralysis and other symptoms of cerebral arterial insufficiency, but the exact relationship of these reactions to the drug has not been established.

Isolated cases of neuroleptic malignant syndrome have been reported both with and without concomitant use of psychotropic drugs.

Digestive System: Nausea, vomiting, gastric distress and abdominal pain, diarrhea, constipation, anorexia, and dryness of the mouth and pharynx, including glossitis and stomatitis.

Eyes: Scattered punctate cortical lens opacities, increased intraocular pressure as well as conjunctivitis, have been reported. Although a direct causal relationship has not been established, many phenothiazines and related drugs have been shown to cause eye changes.

Musculoskeletal System: Aching joints and muscles, and leg cramps.

Metabolism: Fever and chills. Inappropriate antidiuretic hormone (ADH) secretion syndrome has been reported. Cases of frank water intoxication, with decreased serum sodium (hyponatremia) and confusion, have been reported in association with Carbamazepine use (see PRECAUTIONS, Laboratory Tests). Decreased levels of plasma calcium leading to osteoporosis have been reported.

Other: Multiorgan hypersensitivity reactions occurring days to weeks or months after initiating treatment have been reported in rare cases. Signs or symptoms may include, but are not limited to fever, skin rashes, vasculitis, lymphadenopathy, disorders mimicking lymphoma, arthralgia, leukopenia, eosinophilia, hepatosplenomegaly and abnormal liver function tests. These signs and symptoms may occur in various combinations and not necessarily concurrently. Signs and symptoms may initially be mild. Various organs, including but not limited to, liver, skin, immune system, lungs, kidneys, pancreas, myocardium, and colon may be affected (see PRECAUTIONS, General and PRECAUTIONS, Information for Patients).

Isolated cases of a lupus erythematosus-like syndrome have been reported. There have been occasional reports of elevated levels of cholesterol, HDL cholesterol, and triglycerides in patients taking anticonvulsants.

A case of aseptic meningitis, accompanied by myoclonus and peripheral eosinophilia, has been reported in a patient taking Carbamazepine in combination with other medications. The patient was successfully dechallenged, and the meningitis reappeared upon rechallenge with Carbamazepine.

Drug Abuse and Dependence

No evidence of abuse potential has been associated with Carbamazepine, nor is there evidence of psychological or physical dependence in humans.

Overdosage

Acute Toxicity

Lowest known lethal dose: adults, 3.2 g (a 24-year-old woman died of a cardiac arrest and a 24-year-old man died of pneumonia and hypoxic encephalopathy); children, 4 g (a 14-year-old girl died of a cardiac arrest), 1.6 g (a 3-year-old girl died of aspiration pneumonia).

Oral LD50 in animals (mg/kg): mice, 1100 to 3750; rats, 3850 to 4025; rabbits, 1500 to 2680; guinea pigs, 920.

Signs and Symptoms

The first signs and symptoms appear after 1 to 3 hours. Neuromuscular disturbances are the most prominent. Cardiovascular disorders are generally milder, and severe cardiac complications occur only when very high doses (> 60 g) have been ingested.

Respiration: Irregular breathing, respiratory depression.

Cardiovascular System: Tachycardia, hypotension or hypertension, shock, conduction disorders.

Nervous System and Muscles: Impairment of consciousness ranging in severity to deep coma. Convulsions, especially in small children. Motor restlessness, muscular twitching, tremor, athetoid movements, opisthotonos, ataxia, drowsiness, dizziness, mydriasis, nystagmus, adiadochokinesia, ballism, psychomotor disturbances, dysmetria. Initial hyperreflexia, followed by hyporeflexia.

Gastrointestinal Tract: Nausea, vomiting.

Kidneys and Bladder: Anuria or oliguria, urinary retention.

Laboratory Findings: Isolated instances of overdosage have included leukocytosis, reduced leukocyte count, glycosuria, and acetonuria. EEG may show dysrhythmias.

Combined Poisoning: When alcohol, tricyclic antidepressants, barbiturates, or hydantoins are taken at the same time, the signs and

Hylira Gel

Pronunciation: SOE-dee-um hye-a-loo-ROE-nate
Generic Name: Sodium Hyaluronate
Brand Name: Hylira

Hylira Gel is used for:

Treating dry, scaly skin.

Hylira Gel is a mucopolysaccharide. It works by replacing a substance found in the skin.

Do NOT use Hylira Gel if:

you are allergic to any ingredient in Hylira Gel

Contact your doctor or health care provider right away if any of these apply to you.

Before using Hylira Gel:

Some medical conditions may interact with Hylira Gel. Tell your doctor or pharmacist if you have any medical conditions, especially if any of the following apply to you:

if you are pregnant, planning to become pregnant, or are breast-feeding

if you are taking any prescription or nonprescription medicine, herbal preparation, or dietary supplement

if you have allergies to medicines, foods, or other substances

Some MEDICINES MAY INTERACT with Hylira Gel. Because little, if any, of Hylira Gel is absorbed into the blood, the risk of it interacting with another medicine is low.

This may not be a complete list of all interactions that may occur. Ask your health care provider if Hylira Gel may interact with other medicines that you take. Check with your health care provider before you start, stop, or change the dose of any medicine.

How to use Hylira Gel:

Use Hylira Gel as directed by your doctor. Check the label on the medicine for exact dosing instructions.

Wash your hands before and after using Hylira Gel, unless your hands are part of the treated area.

Apply a generous amount of medicine to the affected area and rub in well.

If you miss a dose of Hylira Gel, use it as soon as possible. If it is almost time for your next dose, skip the missed dose and go back to your regular dosing schedule. Do not use 2 doses at once.

Ask your health care provider any questions you may have about how to use Hylira Gel.

Important safety information:

Hylira Gel is for external use only. Do not get Hylira Gel in your eyes, nose, or mouth. If you get Hylira Gel in your eyes, rinse with cool water right away.

Do not use Hylira Gel for other skin conditions at a later time.

PREGNANCY and BREAST-FEEDING: It is unknown if Hylira Gel can cause harm to the fetus. If you become pregnant while taking Hylira Gel, discuss with your doctor the benefits and risks of using Hylira Gel during pregnancy. It is unknown if Hylira Gel is excreted in breast milk. If you are or will be breast-feeding while you are using Hylira Gel, check with your doctor to discuss the risks to your baby.

Possible side effects of Hylira Gel:

All medicines may cause side effects, but many people have no, or minor, side effects. No COMMON side effects have been reported with Hylira Gel. Seek medical attention right away if any of these SEVERE side effects occur:

Severe allergic reactions (rash; hives; difficulty breathing; tightness in the chest; swelling of the mouth, face, lips, or tongue).

This is not a complete list of all side effects that may occur. If you have questions about side effects, contact your health care provider. Call your doctor for medical advice about side effects. To report side effects to the appropriate agency, please read the Guide to Reporting Problems to FDA.

See also: Hylira side effects (in more detail)

If OVERDOSE is suspected:

Contact 1-800-222-1222 (the American Association of Poison Control Centers), your local poison control center (http://www.aapcc.org ), or emergency room immediately.

Proper storage of Hylira Gel:

Store Hylira Gel at room temperature, between 59 and 86 degrees F (15 and 30 degrees C). Store away from heat, moisture, and light. Keep Hylira Gel out of the reach of children and away from pets.

General information:

If you have any questions about Hylira Gel, please talk with your doctor, pharmacist, or other health care provider.

Hylira Gel is to be used only by the patient for whom it is prescribed. Do not share it with other people.

If your symptoms do not improve or if they become worse, check with your doctor.

Check with your pharmacist about how to dispose of unused medicine.

This information is a summary only. It does not contain all information about Hylira Gel. If you have questions about the medicine you are taking or would like more information, check with your doctor, pharmacist, or other health care provider.

Issue Date: February 1, 2012

Database Edition 12.1.1.002

More Hylira resources

Hylira Side Effects (in more detail)
Hylira Use in Pregnancy & Breastfeeding
Hylira Support Group
1 Review for Hylira - Add your own review/rating

Compare Hylira with other medications

Burns, External
Dermatitis
Dermatologic Lesion
Dermatological Disorders

Sunday, November 13, 2016

Camphor Patch

Pronunciation: KAM-for/METH-il sa-LIS-i-late/MEN-thol
Generic Name: Camphor
Brand Name: DuraProxin ES

Camphor Patch is used for:

Temporary relief of minor muscle and joint aches and pains caused by arthritis, simple backache, strains, sprains, and bruises. It may also be used for other conditions as determined by your doctor.

Camphor Patch is a topical analgesic. It works by temporarily relieving minor pain.

Do NOT use Camphor Patch if:

you are allergic to any ingredient in Camphor Patch, including oil of wintergreen

Contact your doctor or health care provider right away if any of these apply to you.

Before using Camphor Patch:

Some medical conditions may interact with Camphor Patch. Tell your doctor or pharmacist if you have any medical conditions, especially if any of the following apply to you:

if you are pregnant, planning to become pregnant, or are breast-feeding

if you are taking any prescription or nonprescription medicine, herbal preparation, or dietary supplement

if you have allergies to medicines, foods, or other substances

if you have had an allergic reaction to aspirin or other salicylates

if you have a wound at the affected area or your skin is broken, reddened, or damaged in any way

Some MEDICINES MAY INTERACT with Camphor Patch. Tell your health care provider if you are taking any other medicines, especially any of the following:

Anticoagulants (eg, warfarin) because the risk of their side effects may be increased by Camphor Patch

This may not be a complete list of all interactions that may occur. Ask your health care provider if Camphor Patch may interact with other medicines that you take. Check with your health care provider before you start, stop, or change the dose of any medicine.

How to use Camphor Patch:

Use Camphor Patch as directed by your doctor. Check the label on the medicine for exact dosing instructions.

Camphor Patch is only to be used on intact, clean, dry skin. Do not apply Camphor Patch to wounds or damaged skin.

Open pouch and remove patch. If needed, cut patch to size. Peel off protective backing and apply the sticky side to the affected area.

Wash your hands immediately after using Camphor Patch.

Do not bandage tightly after applying Camphor Patch.

Do not use Camphor Patch more often than 3 to 4 times per day.

If you miss a dose of Camphor Patch and you are using it regularly, use it as soon as possible. If several hours have passed or if it is nearing time for the next dose, do not double the dose to catch up, unless advised by your health care provider. Do not use 2 doses at once.

Ask your health care provider any questions you may have about how to use Camphor Patch.

Important safety information:

Camphor Patch is for external use only. Avoid contact with your eyes, ears, lips, mouth, or genital area. If you get it in any of these areas, rinse right away with cool water.

Do not use a heating pad after you apply Camphor Patch.

Do NOT use more than the recommended dose or use more often than directed without checking with your doctor.

If your symptoms do not get better within 7 days, if they get worse, or if they get better and then return, check with your doctor.

Camphor Patch has a salicylate in it. Salicylates have been linked to a serious illness called Reye syndrome. Do not give Camphor Patch to a child or teenager who has the flu, chickenpox, or a viral infection. Contact your doctor with any questions or concerns

Camphor Patch may cause harm if it is swallowed. If you may have taken it by mouth, contact your poison control center or emergency room right away.

Camphor Patch should not be used in CHILDREN younger than 12 years old without first checking with the child's doctor; safety and effectiveness in these children have not been confirmed.

PREGNANCY and BREAST-FEEDING: If you become pregnant, contact your doctor. You will need to discuss the benefits and risks of using Camphor Patch while you are pregnant. It is not known if Camphor Patch is found in breast milk after topical use. If you are or will be breast-feeding while you use Camphor Patch, check with your doctor. Discuss any possible risks to your baby.

Possible side effects of Camphor Patch:

All medicines may cause side effects, but many people have no, or minor, side effects. No COMMON side effects have been reported with Camphor Patch. Seek medical attention right away if any of these SEVERE side effects occur:

Severe allergic reactions (rash; hives; itching; difficulty breathing; tightness in the chest; swelling of the mouth, face, lips, or tongue); skin redness or irritation.

If OVERDOSE is suspected:

Contact 1-800-222-1222 (the American Association of Poison Control Centers), your local poison control center, or emergency room immediately.

Proper storage of Camphor Patch:

Store Camphor Patch at room temperature, between 59 and 68 degrees F (15 and 20 degrees C). Store away from heat and light. Do not store in the bathroom. Keep Camphor Patch out of the reach of children and away from pets.

General information:

If you have any questions about Camphor Patch, please talk with your doctor, pharmacist, or other health care provider.

Camphor Patch is to be used only by the patient for whom it is prescribed. Do not share it with other people.

If your symptoms do not improve or if they become worse, check with your doctor.

Check with your pharmacist about how to dispose of unused medicine.

This information is a summary only. It does not contain all information about Camphor Patch. If you have questions about the medicine you are taking or would like more information, check with your doctor, pharmacist, or other health care provider.

Issue Date: February 1, 2012

Database Edition 12.1.1.002

Rimso-50

dimethyl sulfoxide

Dosage Form: irrigation
Rimso-50®

brand of dimethyl sulfoxide irrigation, USP

PRESCRIBING INFORMATION

Rimso-50 Description

Rimso-50®, brand of dimethyl sulfoxide (DMSO) 50% w/w Aqueous Solution for intravesical instillation.

Each mL contains 0.54 gm dimethyl sulfoxide STERILE AND NON-PYROGENIC.

Intravesical instillation for the treatment of interstitial cystitis.

NOT FOR I.M. OR I.V. INJECTION.

Rx only.

The active component of Rimso-50® is dimethyl sulfoxide which has the empirical formula C2H6OS, and is structurally represented as:

Dimethyl sulfoxide is a clear, colorless and essentially odorless liquid which is miscible with water and most organic solvents. Other physical characteristics include: molecular weight 78.13, melting point 18.3° C, and a specific gravity of 1.096.

Rimso-50 - Clinical Pharmacology

Dimethyl sulfoxide is metabolised in man by oxidation to dimethyl sulfone or by reduction to dimethyl sulfide. Dimethyl sulfoxide and dimethyl sulfone are excreted in the urine and feces. Dimethyl sulfide is eliminated through the breath and skin and is responsible for the characteristic odor from patients on dimethyl sulfoxide medication. Dimethyl sulfone can persist in serum for longer than two weeks after a single intravesical instillation. No residual accumulation of dimethyl sulfoxide has occurred in man or lower animals who have received treatment for protracted periods of time. Following topical application, dimethyl sulfoxide is absorbed and generally distributed in the tissues and body fluids.

Indications and Usage for Rimso-50

Rimso-50® (dimethyl sulfoxide) is indicated for the symptomatic relief of patients with interstitial cystitis. Rimso-50® has not been approved as being safe and effective for any other indication. There is no clinical evidence of effectiveness of dimethyl sulfoxide in the treatment of bacterial infections of the urinary tract.

Contraindications

None known.

Warnings

Dimethyl sulfoxide can initiate the liberation of histamine and there has been occasional hypersensitivity reaction with topical administration of dimethyl sulfoxide. This hypersensitivity has been reported in one patients receiving intravesical Rimso-50®. The physician should be cognizant of this possibility in prescribing Rimso-50®. If anaphylactoid symptoms develop, appropriate therapy should be instituted.

Precautions

Changes in the refractive index and lens opacities have been seen in monkeys, dogs and rabbits given high doses of dimethyl sulfoxide chronically. Since lens changes were noted in animals, full eye evaluations, including slit lamp examinations, are recommended prior to and periodically during treatment.

Approximately every six months patients receiving dimethyl sulfoxide should have a biochemical screening, particularly liver and renal function tests, and complete blood count.

Intravesical instillation of Rimso-50® may be harmful to patients with urinary tract malignancy because of dimethyl sulfoxide-induced vasodilation.

Some data indicate that dimethyl sulfoxide potentiates other concomitantly administered medications.

Pregnancy Category C

Dimethyl sulfoxide caused teratogenic responses in hamsters, rats and mice when administered intraperitoneally at high doses (2.5 to 12 gm/kg). Oral or topical doses of dimethyl sulfoxide did not cause problems of reproduction in rats, mice and hamsters. Topical doses (5 gm/kg first two days, then 2.5 gm/kg - last eight days) produced terata in rabbits, but in another study, topical doses of 1.1 gm/kg days 3 through 16 of gestation failed to produce any abnormalities. There are no adequate and well controlled studies in pregnant women. Dimethyl sulfoxide should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus.

INFORMATION FOR PATIENTS (Patient Copy)

Rimso-50® is a sterile solution of 50% dimethyl sulfoxide (DMSO) and 50% water that has been approved by the U.S. Food and Drug Administration for use in the symptomatic relief of patients with interstitial cystitis.

Rimso-50® will be instilled in the bladder on an inpatient or out-patient basis, which will be determined by your physician.

Some data indicate that dimethyl sulfoxide could change the effectiveness of medication(s) that you may be presently receiving. Be sure to mention the name and dosage of all medicines you are taking to your physician before a Rimso-50® instillation.

A garlic-like taste may be noted by the patient within a few minutes after instillation of Rimso-50® (dimethyl sulfoxide). This taste may last several hours. An odor on the breath and skin may be present and remain for up to 72 hours.

Some patients may experience discomfort on administration of the drug. Usually this becomes less prominent with repeated administration.

If you are pregnant or nursing, ask your physician about the advisability of using Rimso-50®.

Some eye changes have been observed in animals treated with DMSO in large doses for prolonged periods. Therefore your doctor may want you to have eye evaluations, including slit lamp examinations prior to and periodically during treatment.

It is not known whether this drug is excreted in human milk. Because many drugs are excreted in human milk, caution should be exercised when dimethyl sulfoxide is administered to a nursing woman.

Safety and effectiveness in children have not been established.

Information available to be given to the patient is reprinted at the end of this text.

Adverse Reactions

A garlic-like taste may be noted by the patient within a few minutes after instillation of Rimso-50® (dimethyl sulfoxide). This taste may last several hours and because of the presence of metabolites, an odor on the breath and skin may remain for 72 hours.

Transient chemical cystitis has been noted following instillation of dimethyl sulfoxide.

The patient may experience moderately severe discomfort on administration. Usually this becomes less prominent with repeated administration.

Drug Abuse and Dependence

None known.

Overdosage

The oral LD50 of dimethyl sulfoxide in the dog is greater than 10 gm/kg. It is improbable that this dosage level could be obtained with intravesical instillation of Rimso-50® in the patient.

In case of accidental oral ingestion, specific measures should be taken to induce emesis. Additional measures which may be considered are gastric lavage, activated charcoal and force diuresis.

Rimso-50 Dosage and Administration

Instillation of 50 mL of Rimso-50® (dimethyl sulfoxide) directly into the bladder may be accomplished by catheter or asepto syringe and allow to remain for 15 minutes. Application of an analgesic lubricant gel such as lidocaine jelly to the urethra is suggested prior to insertion of the catheter to avoid spasm. The medication is expelled by spontaneous voiding. It is recommended that the treatment be repeated every two weeks until maximum symptomatic relief is obtained. Thereafter, time intervals between therapy may be increased appropriately.

Administration of oral analgesic medication or suppositories containing belladonna and opium prior to the instillation of Rimso-50® can reduce bladder spasm.

In patients with severe interstitial cystitis with very sensitive bladders, the initial treatment, and possibly the second and third (depending on patient response) should be done under anesthesia. (Saddle block has been suggested).

How is Rimso-50 Supplied

Bottles contain 50 mL of sterile and non-pyrogenic Rimso-50® (50% w/w dimethyl sulfoxide aqueous solution).

Dimethyl sulfoxide is clear and colorless.

Protect from strong light.

Store at room temperature (59° to 86°F) (15° to 30°C).

NDC #67457-177-50.

For additional information concerning Rimso-50®, contact Bioniche Pharma USA LLC, Lake Forest, IL 60045

Manufactured for: Bioniche Pharma USA LLC, Lake Forest, IL 60045

Manufactured by: Bioniche Teo., Inverin, Co. Galway, Ireland.

INFORMATION FOR PATIENTS (Physician Copy)

Rimso-50® will be instilled in the bladder on an inpatient or out-patient basis, which will be determined by your physician.

Some patients may experience discomfort on administration of the drug. Usually this becomes less prominent with repeated administration.

If you are pregnant or nursing, ask your physician about the advisability of using Rimso-50®.

Bioniche Pharma USA LLC,

Lake Forest, IL 60045

0582L100

PRINCIPAL DISPLAY PANEL - 50 mL Vial

Rimso-50®

brand of

dimethyl sulfoxide

irrigation, USP

STERILE AND NON-PYROGENIC

Rx only.

Manufactured for: Bioniche Pharma USA LLC, Lake Forest, IL 60045

Manufactured by: Bioniche Teo., Inverin, Co. Galway, Ireland.

Rimso-50
dimethyl sulfoxide irrigant

Product Information
Product Type	HUMAN PRESCRIPTION DRUG	NDC Product Code (Source)	67457-177
Route of Administration	INTRAVESICAL	DEA Schedule

Active Ingredient/Active Moiety
Ingredient Name	Basis of Strength	Strength
Dimethyl Sulfoxide (Dimethyl Sulfoxide)	Dimethyl Sulfoxide	0.54 g in 1 mL

Inactive Ingredients
Ingredient Name	Strength
WATER

Product Characteristics
Color		Score
Shape		Size
Flavor		Imprint Code
Contains

Packaging
#	NDC	Package Description	Multilevel Packaging
1	67457-177-50	1 VIAL In 1 CARTON	contains a VIAL, GLASS
1		50 mL In 1 VIAL, GLASS	This package is contained within the CARTON (67457-177-50)

Marketing Information
Marketing Category	Application Number or Monograph Citation	Marketing Start Date	Marketing End Date
NDA	NDA017788	04/01/1978

Labeler - Bioniche Pharma USA LLC (790384503)

Establishment
Name	Address	ID/FEI	Operations
Bioniche Teoranta		896321325	MANUFACTURE

Revised: 11/2009Bioniche Pharma USA LLC

More Rimso-50 resources

Rimso-50 Side Effects (in more detail)
Rimso-50 Use in Pregnancy & Breastfeeding
Rimso-50 Drug Interactions
Rimso-50 Support Group
0 Reviews for Rimso-50 - Add your own review/rating

Rimso-50 Concise Consumer Information (Cerner Multum)

Rimso-50 Advanced Consumer (Micromedex) - Includes Dosage Information

Dimethyl Sulfoxide MedFacts Consumer Leaflet (Wolters Kluwer)

Compare Rimso-50 with other medications

Interstitial Cystitis

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid

Pronunciation: klor-fen-EER-a-meen/dex-troe-meth-OR-fan/fen-ill-EF-rin
Generic Name: Chlorpheniramine/Dextromethorphan/Phenylephrine
Brand Name: Examples include Poly-Tussin DM and Ceron-DM

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid is used for:

Relieving sinus congestion, runny nose, sneezing, and cough due to colds, upper respiratory infections, and allergies. It may also be used for other conditions as determined by your doctor.

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid is a decongestant, antihistamine, and cough suppressant combination. It works by constricting blood vessels and reducing swelling in the nasal passages. The antihistamine works by blocking histamine, which helps reduce symptoms, such as watery eyes and sneezing, while the cough suppressant works in the brain to help decrease the cough reflex.

Do NOT use Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid if:

you are allergic to any ingredient in Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid

you have severe high blood pressure, severe heart blood vessel disease, rapid heartbeat, or severe heart problems

you are unable to urinate or are having an asthma attack

you take sodium oxybate (GHB) or you have taken furazolidone or a monoamine oxidase (MAO) inhibitor (eg, phenelzine) within the last 14 days

Contact your doctor or health care provider right away if any of these apply to you.

Before using Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid:

Some medical conditions may interact with Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid. Tell your doctor or pharmacist if you have any medical conditions, especially if any of the following apply to you:

if you are pregnant, plan to become pregnant, or are breast-feeding

if you are taking any prescription or nonprescription medicine, herbal preparation, or dietary supplement

if you have allergies to medicines, foods, or other substances

if you have a fast, slow, or irregular heartbeat

if you have a history of adrenal gland problems (eg, tumor); heart problems; high blood pressure; diabetes; heart blood vessel problems; stroke; glaucoma; a blockage of your stomach, intestines, or bladder; ulcers; trouble urinating; an enlarged prostate or other prostate problems; seizures; or an overactive thyroid

if you have a history of asthma, chronic cough, chronic obstructive pulmonary disease (COPD), or other lung problems (eg, chronic bronchitis, emphysema), or if your cough produces large amounts of mucus

Some MEDICINES MAY INTERACT with Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid. Tell your health care provider if you are taking any other medicines, especially any of the following:

Beta-blockers (eg, propranolol), COMT inhibitors (eg, tolcapone), furazolidone, indomethacin, MAO inhibitors (eg, phenelzine), sodium oxybate (GHB), or tricyclic antidepressants (eg, amitriptyline) because side effects of Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid may be increased

Digoxin or droxidopa because the risk of irregular heartbeat or heart attack may be increased

Bromocriptine or hydantoins (eg, phenytoin) because side effects may be increased by Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid

Guanadrel, guanethidine, methyldopa, mecamylamine, or reserpine because their effectiveness may be decreased by Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid

This may not be a complete list of all interactions that may occur. Ask your health care provider if Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid may interact with other medicines that you take. Check with your health care provider before you start, stop, or change the dose of any medicine.

How to use Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid:

Use Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid as directed by your doctor. Check the label on the medicine for exact dosing instructions.

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid may be taken with or without food.

Use a measuring device marked for medicine dosing. Ask your pharmacist for help if you are unsure of how to measure your dose.

If you miss a dose of Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid, take it as soon as possible. If it is almost time for your next dose, skip the missed dose and go back to your regular dosing schedule. Do not take 2 doses at once.

Ask your health care provider any questions you may have about how to use Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid.

Important safety information:

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid may cause dizziness, drowsiness, or blurred vision. Do not drive, operate machinery, or do anything else that could be dangerous until you know how you react to Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid. Using Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid alone, with certain other medicines, or with alcohol may lessen your ability to drive or perform other potentially dangerous tasks.

Do not take diet or appetite control medicines while you are taking Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid without checking with your doctor.

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid contains phenylephrine. Before you begin taking any new prescription or nonprescription medicine, read the ingredients to see if it also contains phenylephrine. If it does or if you are uncertain, contact your doctor or pharmacist.

Do NOT exceed the recommended dose or take Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid for longer than prescribed without checking with your doctor.

If your symptoms do not improve within 5 to 7 days or if they become worse, check with your doctor.

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid may cause increased sensitivity to the sun. Avoid exposure to the sun, sunlamps, or tanning booths until you know how you react to Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid. Use a sunscreen or protective clothing if you must be outside for a prolonged period.

If you are scheduled for allergy skin testing, do not take Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid for several days before the test because it may decrease your response to the skin tests.

Before you have any medical or dental treatments, emergency care, or surgery, tell the doctor or dentist that you are using Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid.

Use Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid with caution in the ELDERLY because they may be more sensitive to its effects.

Caution is advised when using Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid in CHILDREN because they may be more sensitive to its effects.

PREGNANCY and BREAST-FEEDING: If you become pregnant while taking Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid, discuss with your doctor the benefits and risks of using Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid during pregnancy. It is unknown if Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid is excreted in breast milk. Do not breast-feed while taking Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid.

Possible side effects of Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid:

All medicines may cause side effects, but many people have no, or minor, side effects. Check with your doctor if any of these most COMMON side effects persist or become bothersome:

Constipation; diarrhea; dizziness; drowsiness; excitability; headache; loss of appetite; nausea; nervousness or anxiety; trouble sleeping; upset stomach; vomiting; weakness.

Seek medical attention right away if any of these SEVERE side effects occur:

Severe allergic reactions (rash; hives; difficulty breathing; tightness in the chest; swelling of the mouth, face, lips, or tongue); difficulty urinating or inability to urinate; fast or irregular heartbeat; hallucinations; seizures; severe dizziness, lightheadedness, or headache; tremor; trouble sleeping; vision changes.

This is not a complete list of all side effects that may occur. If you have questions about side effects, contact your health care provider. Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800-FDA-1088. You may also report side effects at http://www.fda.gov/medwatch .

See also: Chlorpheniramine/Dextromethorphan/Phenylephrine side effects (in more detail)

If OVERDOSE is suspected:

Contact 1-800-222-1222 (the American Association of Poison Control Centers), your local poison control center, or emergency room immediately. Symptoms may include blurred vision; confusion; hallucinations; severe dizziness, lightheadedness, or headache; severe drowsiness; seizures; unusually fast, slow, or irregular heartbeat; vomiting.

Proper storage of Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid:

Store Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid at room temperature, between 59 and 86 degrees F (15 and 30 degrees C). Store away from heat, moisture, and light. Do not store in the bathroom. Keep Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid out of the reach of children and away from pets.

General information:

If you have any questions about Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid, please talk with your doctor, pharmacist, or other health care provider.

Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid is to be used only by the patient for whom it is prescribed. Do not share it with other people.

If your symptoms do not improve or if they become worse, check with your doctor.

Check with your pharmacist about how to dispose of unused medicine.

This information is a summary only. It does not contain all information about Chlorpheniramine/Dextromethorphan/Phenylephrine Liquid. If you have questions about the medicine you are taking or would like more information, check with your doctor, pharmacist, or other health care provider.

Issue Date: February 1, 2012

Database Edition 12.1.1.002

More Chlorpheniramine/Dextromethorphan/Phenylephrine resources

Chlorpheniramine/Dextromethorphan/Phenylephrine Side Effects (in more detail)
Chlorpheniramine/Dextromethorphan/Phenylephrine Use in Pregnancy & Breastfeeding
Chlorpheniramine/Dextromethorphan/Phenylephrine Drug Interactions
Chlorpheniramine/Dextromethorphan/Phenylephrine Support Group
6 Reviews for Chlorpheniramine/Dextromethorphan/Phenylephrine - Add your own review/rating

Compare Chlorpheniramine/Dextromethorphan/Phenylephrine with other medications

Cough and Nasal Congestion

Saturday, November 12, 2016

Codeine

Class: Opiate Agonists
Note: This monograph also contains information on Codeine Phosphate, Codeine Sulfate
VA Class: CN101
Chemical Name: (5α,6α)-7,8-Didehydro-4,5-epoxy-3-methoxy-17-methyl-morphan-6-ol monohydrate
Molecular Formula: C₁₈H₂₁NO₃•H₂OC₁₈H₂₁NO₃•H₃PO₄•½H₂O
CAS Number: 6059-47-8
Brands: Ambenyl, Bromanyl, BenzaClin, Brontex, Capital and Codeine, Cheracol with Codeine, Codimal PH, Colrex Compound, Cycofed Expectorant Pediatric, Decohistine DH, Dihistine DH Elixir, Duac, Fioricet with Codeine, Fiorinal with Codeine, Gani-Tuss NR, Guiatuss AC, Guiatussin with Codeine, HaNew Riversin, KG-Fed Pediatric Expectorant, Mytussin AC, Novahistine DH, Nucofed, Nucotuss Pediatric, Pediacof, Phenergan VC with Codeine, Phenhist DH with Codeine Modified Formula, Prometh VC with Codeine Phosphate, Robafen AC, Robitussin A-C, Ryna-C, Ryna-CX, Soma Compound with Codeine, Triacin-C, Tussar SF, Tussar-2 Syrup, Tussi-Organidin NR, Tussi-Organidin-S NR, Tylenol with Codeine

Introduction

Opiate agonist; phenanthrene derivative.^a ^b

Uses for Codeine

Pain

Symptomatic relief of mild to moderate pain that is not relieved by a non-opiate analgesic.^b ^d ^e ^f

Combinations of codeine and aspirin or acetaminophen may produce additive analgesic effects because of differing mechanisms of action.^b

Cough

Symptomatic relief of nonproductive cough, alone or in combination with other antitussives or expectorants.^a

Codeine Dosage and Administration

Administration

Oral Administration

Administer orally.^a ^b

Dispense a calibrated measuring device with cough preparations intended for children 2–5 years of age.¹⁰³

Dosage

Available as codeine phosphate and codeine sulfate; dosage expressed in terms of the salt.^d ^e ^g

Pediatric Patients

Cough

Oral

Usual Pediatric Antitussive Dosages
Age	Daily Dosage
2–5 years	1 mg/kg daily in 4 equally divided doses every 4–6 hours¹⁰⁰ ¹⁰¹ ¹⁰³
6–11 years	5–10 mg every 4–6 hours¹⁰⁰ ¹⁰¹ ¹⁰³
≥12 years	10–20 mg every 4–6 hours^a

Alternatively, use the following dosages as a guide based on average body weight; reduce dosage for low-weight children.¹⁰⁰

Antitussive Dosages for Pediatric Patients Based on Weight100
Age	Daily Dosage
2 years (averaging 12 kg)	3 mg every 4–6 hours (maximum 12 mg daily)
3 years (averaging 14 kg)	3.5 mg every 4–6 hours (maximum 14 mg daily)
4 years (averaging 16 kg)	4 mg every 4–6 hours (maximum 16 mg daily)
5 years (averaging 18 kg)	4.5 mg every 4–6 hours (maximum 18 mg daily)

Pain

Oral

3 mg/kg or 100 mg/m² daily in 6 divided doses.^b Alternatively, 0.5 mg/kg or 15 mg/m² every 4–6 hours.^b ^f

Adults

Cough

Oral

10–20 mg every 4–6 hours.^a

Pain

Oral

30 mg every 4 hours as needed; usual dosage range is 15–60 mg every 4 hours as needed.^b ^d ^e

Nonopiate-containing analgesic fixed combinations: Nonopiate component may limit dosage of opiate component.¹¹⁷ ¹¹⁹ ¹²⁰ ¹²¹ Nonopiate analgesics are available in various fixed ratios with codeine and also are available in many other prescription and OTC preparations; ensure that therapy is not duplicated and that nonopiate dosage does not exceed maximum recommended dosages.¹¹⁷ ¹¹⁸ ¹¹⁹ ¹²¹

Prescribing Limits

Pediatric Patients

Cough

Oral

Maximum Daily Antitussive Dosages for Pediatric Patients
Age	Maximum Daily Dosage
2 years (averaging 12 kg)	12 mg¹⁰⁰
3 years (averaging 14 kg)	14 mg ¹⁰⁰
4 years (averaging 16 kg)	16 mg ¹⁰⁰
5 years (averaging 18 kg)	18 mg ¹⁰⁰
6–11 years	60 mg ^a
≥12 years	120 mg ^a

Adults

Cough

Oral

Maximum 120 mg daily.^a

Special Populations

Geriatric Patients

Reduce dosage in older patients.^a ^b

Ultra-rapid Metabolizers of CYP2D6 Substrates

Use lowest effective dosage for shortest period of time.¹⁰⁴ ¹⁰⁵ ¹⁰⁶ ¹¹³ (See Special Populations under Pharmacokinetics.)

Cautions for Codeine

Contraindications

Known hypersensitivity to codeine or any ingredient in the formulation.^c ^d ^e ^f

Warnings/Precautions

Warnings

CNS Depression

Performance of activities requiring mental alertness and physical coordination may be impaired.^a ^c ^d ^e ^f

Concurrent use of other CNS depressants may potentiate CNS depression.^d ^e (See Specific Drugs under Interactions.)

Abuse Potential

Possible tolerance, psychologic dependence, and physical dependence following prolonged administration.^a Abuse potential similar to that of morphine.^d ^e ^f

Sulfite Sensitivity

Some formulations contain sulfites, which may cause allergic-type reactions (including anaphylaxis and life-threatening or less severe asthmatic episodes) in certain susceptible individuals.^f

General Precautions

Increased Intracranial Pressure or Head Trauma

Potential for increased respiratory depressant effects and elevation of CSF pressure in patients with increased intracranial pressure, head trauma, or other intracranial lesions.^c ^d ^e ^f

Adverse effects of opiates may obscure the existence, extent, or course of intracranial pathology.^d ^e ^f ^g

Acute Abdominal Conditions

Administration may complicate assessment of patients with acute abdominal conditions.^c ^d ^e ^f

Respiratory Depression

Possible dose-related respiratory depression^c ^d ^e (occurs infrequently with oral antitussive doses).^a

Potential for increased viscosity of bronchial secretions and suppression of cough reflex, with subsequent respiratory insufficiency, in patients with asthma or pulmonary emphysema who indiscriminately use antitussives.^a

Postoperative Patients

Suppression of cough reflex following thoracotomy or laparotomy may lead to postoperative retention of secretions; cautious use recommended.^a

Debilitated and Special Risk Patients

Use with caution in debilitated patients and in those with hypothyroidism, Addison’s disease, and prostatic hypertrophy or urethral stricture.^a ^d ^e ^f

Fixed-combination Preparations

When used in fixed combination with other drug(s), consider the cautions, precautions, and contraindications associated with the other drug(s).^b

Specific Populations

Pregnancy

Category C.^f

Lactation

Distributed into milk. ^a Use with caution in nursing women who are known or suspected ultra-rapid metabolizers of CYP2D6 substrates; opioid toxicity resulting in neonatal death reported in the nursing infant of mother receiving codeine; mother was an ultra-rapid metabolizer of codeine.¹⁰⁴ ¹⁰⁵ ¹⁰⁶ ¹⁰⁷ ¹¹³ (See Metabolism and see Special Populations under Pharmacokinetics.)

The FDA-approved AmpliChip CYP450 Test can be used to identify CYP2D6 genotype.¹⁰⁶ ¹¹¹ ¹¹³ Testing alone may not adequately predict risk of adverse reactions and should not substitute for clinical judgment.¹⁰⁴ If codeine is used in nursing women, administer lowest effective dosage for shortest possible time; closely monitor for opioid toxicity in both mother and infant.¹⁰⁴ ¹⁰⁵ ¹⁰⁶ ¹¹³

Pediatric Use

Safety for the management of mild to moderate pain not established in children <3 years of age.^d ^e ^f

Use as antitussive not recommended in children <2 years of age; possible respiratory arrest, coma, and death due to increased susceptibility to respiratory depressant effects.^a

Risk of overdosage and toxicity (including death) in children <2 years of age receiving OTC preparations containing antihistamines, cough suppressants, expectorants, and nasal decongestants alone or in combination for relief of symptoms of upper respiratory tract infection.¹¹⁵ ¹¹⁶ Limited evidence of efficacy for these preparations in this age group; appropriate dosages not established.¹¹⁵ Therefore, FDA recommends not to use such preparations in children <2 years of age; safety and efficacy in older children currently under evaluation. Because children 2–3 years of age also are at increased risk of overdosage and toxicity, some manufacturers of oral nonprescription cough and cold preparations recently agreed to voluntarily revise the product labeling to state that such preparations should not be used in children <4 years of age. During the transition period, some preparations on pharmacy shelves will have the new recommendation (“do not use in children <4 years of age”), while others will have the previous recommendation (“do not use in children <2 years of age”). FDA recommends that parents and caregivers adhere to dosage instructions and warnings on the product labeling that accompanies the preparation and consult a clinician about any concerns. Clinicians should ask caregivers about use of OTC cough/cold preparations to avoid overdosage.

Geriatric Use

Use with caution.^d ^e ^f ^g (See Geriatric Patients under Dosage and Administration.)

Hepatic Impairment

Use with caution in patients with severe hepatic impairment.^d ^e ^f ^g

Renal Impairment

Use with caution in patients with severe renal impairment.^d ^e ^f

Common Adverse Effects

When used for pain relief (particularly in ambulatory patients not experiencing severe pain): lightheadedness, dizziness, sedation, nausea, vomiting, sweating.^d ^e ^f

When used at antitussive doses: nausea, vomiting, constipation (with repeated doses), dizziness, sedation, palpitation, pruritus.^a

Interactions for Codeine

Specific Drugs

Drug	Interaction	Comments
Anticholinergic agents	Possible paralytic ileus^f
Antidepressants, MAO inhibitors and tricyclics	Potentiation of antidepressant effect^c	Use with caution; reduce dosage of codeine^c
CNS depressants (e.g., opiate agonists, general anesthetics, tranquilizers, phenothiazines, sedatives/hypnotics, alcohol)	Additive CNS effects^a ^d ^e ^f	Reduce dosage of one or both agents^d ^e ^f

Codeine Pharmacokinetics

Absorption

Bioavailability

Well absorbed following oral administration.^a ^b ^e ^f ^g

Onset

Onset occurs in 15–30 minutes.^a ^b Peak analgesic effects occur within 2 hours;^g peak antitussive effects within 1–4 hours.ⁱ

Duration

Analgesic effects persist for 4–6 hours.^b ^g Antitussive effects may persist for 4 hours.ⁱ

Distribution

Extent

Rapidly distributed into various body tissues, with preferential uptake by parenchymatous organs such as the liver, spleen, and kidney.^g Distributed into milk.^b Readily crosses the placenta.^c

Protein Binding

Not bound to plasma proteins.^g

Elimination

Metabolism

Metabolized in liver, principally by CYP3A4 and to a lesser extent (10%) by CYP2D6 to O-demethylated morphine, the active metabolite.^b ¹⁰⁸ ¹⁰⁹ ¹¹⁰ ¹¹²

Metabolism of codeine influenced by CYP2D6 polymorphism; genetic differences in drug metabolism affect drug response.¹⁰⁸ ¹⁰⁹ ¹¹⁰ ¹¹² ¹¹⁴ Individuals may be described as poor, extensive, or ultra-rapid metabolizers of CYP2D6 substrates.¹⁰⁸ ¹⁰⁹ ¹¹⁰ ¹¹² ¹¹⁴

Elimination Route

Excreted mainly in urine with negligible amounts of codeine and its metabolites found in feces.^b ^g

Half-life

About 2.5–3 hours.^f ^g

Special Populations

Individuals who carry the genotype associated with ultra-rapid metabolism of CYP2D6 substrates (approximately 1–7% of Caucasians, 10–30% of Ethiopians and Saudi Arabians) convert codeine to morphine more rapidly and completely than other individuals; ultra-rapid metabolizers are likely to have higher than expected serum concentrations of morphine.¹⁰⁷ ¹⁰⁸ ¹¹⁰ ¹¹² ¹¹⁴

Stability

Storage

Oral

Tablets

Tight, light-resistant containers at <40°C (preferably 15–30°C).^b

Solution

Tight, light-resistant containers at <40°C (preferably 15–30°C).^h Protect from freezing.^h

ActionsActions

Principal pharmacologic effects are on CNS and intestines.^c ^d ^e

Mild analgesic effect.^b ^d ^e ^f Acts at several sites within the CNS involving several systems of neurotransmitters to produce analgesia; precise mechanism of action not fully elucidated.^c

Suppresses cough reflex by direct effect on cough center in medulla of brain.^a

Exerts drying effect on respiratory tract mucosa and increases viscosity of bronchial secretions.^a

Antitussive activity is less than that of morphine (on a weight basis).^a

Advice to Patients

Potential for drug to impair mental alertness or physical coordination; use caution when driving or operating machinery until effects on individual are known.^d ^e ^f

Importance of informing clinicians of existing or contemplated concomitant therapy, including prescription and OTC drugs, as well as alcohol consumption and any concomitant diseases.^d ^e ^f Importance of limiting alcohol intake.^f

Importance of women informing their clinician if they are or plan to become pregnant or plan to breast-feed.^d ^e ^f

Risk of morphine toxicity in nursing infants of mothers taking codeine who are ultra-rapid metabolizers of codeine.¹⁰⁴ ¹⁰⁵ ¹⁰⁶ ¹¹³ Importance of monitoring infants for manifestations of morphine overdose (e.g., sedation, difficulty breathing, hypotonia, poor feeding); immediately seek medical attention if any symptoms develop.¹⁰⁴ ¹⁰⁵ ¹¹³

Importance of advising patients of other important precautionary information.^d ^e (See Cautions.)

Preparations

Excipients in commercially available drug preparations may have clinically important effects in some individuals; consult specific product labeling for details.

Subject to control under the Federal Controlled Substances Act of 1970.^d ^e

Codeine
Routes	Dosage Forms	Strengths	Brand Names	Manufacturer
Bulk	Crystals

Codeine Phosphate
Routes	Dosage Forms	Strengths	Brand Names
Bulk	Powder
Oral	Solution	15 mg/5 mL	Codeine Phosphate Oral Solution ( C-II)
	Tablets, soluble	30 mg	Codeine Phosphate Soluble Tablets ( C-II)
		60 mg	Codeine Phosphate Soluble Tablets ( C-II)