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Codeine - Pharmacokinetics |  | Codeine - Pharmacokinetics: Encyclopedia II - Codeine - Pharmacokinetics |  | Codeine is considered a prodrug, since it is metabolised in vivo to the principal active analgesic agent morphine. It is, however, less potent than morphine since only about 10% of the codeine is converted. It also has a correspondingly lower dependence-liability than morphine.
Theoretically, a dose of approximately 200 mg (oral) of codeine must be administered to give equivalent analgesia to 30 mg (oral) of morphine (Rossi, 2004). It is not used, however, in single doses of greater than 60mg (and no more than 240 mg i ...
See also:Codeine, Codeine - Indications, Codeine - Controlled substance, Codeine - Pharmacokinetics, Codeine - Pharmacology, Codeine - Adverse effects, Codeine - Recreational use |  | | Codeine, Codeine - Adverse effects, Codeine - Controlled substance, Codeine - Indications, Codeine - Pharmacokinetics, Codeine - Pharmacology, Codeine - Recreational use, dihydrocodeine, morphine |  | |
|  |  | Codeine: Encyclopedia II - Codeine - Pharmacokinetics
Codeine - Pharmacokinetics
Codeine is considered a prodrug, since it is metabolised in vivo to the principal active analgesic agent morphine. It is, however, less potent than morphine since only about 10% of the codeine is converted. It also has a correspondingly lower dependence-liability than morphine.
Theoretically, a dose of approximately 200 mg (oral) of codeine must be administered to give equivalent analgesia to 30 mg (oral) of morphine (Rossi, 2004). It is not used, however, in single doses of greater than 60mg (and no more than 240 mg in 24 hours) since there is a ceiling effect.
The conversion of codeine to morphine occurs in the liver and is catalysed by the cytochrome P450 enzyme CYP2D6. Approximately 6–10% of the Caucasian population have poorly functional CYP2D6 and codeine is virtually ineffective for analgesia in these patients (Rossi, 2004). Many of the adverse effects, however, are still experienced. Also, some medications are CYP2D6 inhibitors and reduce or even completely eliminate the efficacy of codeine. The most notorious of these are the selective serotonin reuptake inhibitors, such as fluoxetine (Prozac) and citalopram (Celexa).
Other related archivesAlfentanil, Alkaloids, Analgesics, Antitussives, Aspirin, Australia, Buprenorphine, CYP2D6, Canada, Carfentanil, Celecoxib, Class B Drug, Codeine (band), Codeinone, Controlled Substances Act, Cough, Dextropropoxyphene, Diarrhea, Diclofenac, Diflunisal, Dihydrocodeine, Drug Synergy, Fentanyl, France, Heroin, Hydrocodone, Hydromorphone, INN, Ibuprofen, Indomethacin, Ketoprofen, Ketorolac, Meloxicam, Methadone, Misuse of Drugs Act 1971, Morphine, Morphinone, NSAIDs, Naproxen, Natural opium alkaloids, Opiates, Opioids, Oxycodone, Oxymorphone, Paracetamol (acetaminophen), Pethidine (Meperidine), Piroxicam, Remifentanil, Rofecoxib, Schedule II controlled substances, Schedule III controlled substances, Schedule V controlled substances, Single Convention on Narcotic Drugs, Sufentanil, Tetrahydrocannabinol, Tramadol, United Kingdom, United States, Valdecoxib, acetaminophen, alkaloid, analgesic, antitussive, aspirin, blunt, carisoprodol, ceiling effect, citalopram, co-codamol, co-codaprin, cold water extraction, cytochrome P450, dependence, dihydrocodeine, euphoric, extract, fluoxetine, gastrointestinal, hemorrhaging, heroin, ibuprofen, in vivo, kidney, liver, methylation, miosis, morphine, nausea, opioid, opium, orthostatic hypotension, over-the-counter, over-the-counter medication, pain, paracetamol, percent, prescription, prodrug, recreational drug, respiratory depression, selective serotonin reuptake inhibitors, stomach, μ-opioid receptor
 Adapted from the Wikipedia article "Pharmacokinetics", under the G.N U Free Docmentation License. Please also see http://en.wikipedia.org/wiki |
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