Chemistry:Tetrazepam

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Short description: Chemical compound
Tetrazepam
Tetrazepam.svg
Tetrazepam3d.png
Clinical data
AHFS/Drugs.comInternational Drug Names
Routes of
administration
Oral
ATC code
Legal status
Legal status
Pharmacokinetic data
Elimination half-life3–26 hours
Identifiers
CAS Number
PubChem CID
ChemSpider
UNII
KEGG
Chemical and physical data
FormulaC16H17ClN2O
Molar mass288.77 g·mol−1
3D model (JSmol)
  (verify)

Tetrazepam[1] (is marketed under the following brand names, Clinoxan, Epsipam, Myolastan, Musaril, Relaxam and Spasmorelax) is a benzodiazepine derivative with anticonvulsant, anxiolytic, muscle relaxant and slightly hypnotic properties. It was formerly used mainly in Austria, France, Belgium, Germany and Spain to treat muscle spasm, anxiety disorders such as panic attacks, or more rarely to treat depression, premenstrual syndrome or agoraphobia. Tetrazepam has relatively little sedative effect at low doses while still producing useful muscle relaxation and anxiety relief. The Co-ordination Group for Mutual Recognition and Decentralised Procedures-Human (CMD(h)) endorsed the Pharmacovigilance Risk Assessment Committee (PRAC) recommendation to suspend the marketing authorisations of tetrazepam-containing medicines across the European Union (EU) in April 2013.[2] The European Commission has confirmed the suspension of the marketing authorisations for Tetrazepam in Europe because of cutaneous toxicity, effective from the 1 August 2013.[3]

Delayed type 4 allergic hypersensitivity reactions including maculopapular exanthema, erythematous rash, urticarial eruption, erythema multiforme, photodermatitis, eczema and Stevens–Johnson syndrome can occasionally occur as a result of tetrazepam exposure. These hypersensitivity reactions to tetrazepam share no cross-reactivity with other benzodiazepines.[4]

Indications

Tetrazepam is used therapeutically as a muscle relaxant.[5][6]

Availability

The indicated adult dose for muscle spasm is 25 mg to 150 mg per day, increased if necessary to a maximum of 300 mg per day, in divided doses. Tetrazepam is not generally recommended for use in children, except on the advice of a specialist.

Tetrazepam is only available in one strength and formulation, 50 mg tablets. The benzodiazepine equivalent of tetrazepam is approximately 100 mg of tetrazepam = 10 mg of diazepam.[7]

Adverse effects

Allergic reactions to tetrazepam occasionally occur involving the skin.[4]

Allergic reactions can develop to tetrazepam[8][9] and it is considered to be a potential allergen.[10][11] Drug rash and drug-induced eosinophilia with systemic symptoms is a known complication of tetrazepam exposure.[12][13] These hypersensitive allergic reactions can be of the delayed type.[14][15][16]

Toxic epidermal necrolysis has occurred from the use of tetrazepam[17][18] including at least one reported death.[19] Stevens–Johnson syndrome and erythema multiforme has been reported from use of tetrazepam. Cross-reactivity with other benzodiazepines does not typically occur in such patients.[20][21][22] Exanthema[23] and eczema may occur.[24] The lack of cross-reactivity with other benzodiazepines is believed to be due to the molecular structure of tetrazepam.[25][26] Photodermatitis[27] and phototoxicity have also been reported.[28] Occupational contact allergy can also develop from regularly handling tetrazepam.[29][30] Airborne contact dermatitis can also occur as an allergy which can develop from occupational exposure.[31]

Patch test

Patch testing has been used successfully to demonstrate tetrazepam allergy.[32][33] Oral testing can also be used. Skin prick tests are not always accurate and may produce false negatives.[34]

Drowsiness is a common side effect of tetrazepam.[35] A reduction in muscle force can occur.[36] Myasthenia gravis, a condition characterised by severe muscle weakness is another potential adverse effect from tetrazepam.[37] Cardiovascular and respiratory adverse effects can occur with tetrazepam similar to other benzodiazepines.[26]

Tolerance, dependence and withdrawal

Prolonged use, as with all benzodiazepines, should be avoided, as tolerance occurs and there is a risk of benzodiazepine dependence and a benzodiazepine withdrawal syndrome after stopping or reducing dosage.[26]

Overdose

Tetrazepam, like other benzodiazepines is a drug which is very frequently present in cases of overdose. These overdoses are often mixed overdoses, i.e. a mixture of other benzodiazepines or other drug classes with tetrazepam.[38][39]

Contraindications and special caution

Benzodiazepines require special precaution if used in the elderly, during pregnancy, in children, alcohol or drug-dependent individuals and individuals with comorbid psychiatric disorders.[40]

Pharmacology

Tetrazepam is an unusual benzodiazepine in its molecular structure as it has cyclohexenyl group which has substituted the typical 5-phenyl moiety seen in other benzodiazepines.[41] Tetrazepam, is rapidly absorbed after oral administration, within 45 mins and reaches peak plasma levels in less than 2 hours. It is classed as an intermediate acting benzodiazepine with an elimination half-life of approximately 15 hours. It is primarily metabolised to the inactive metabolites 3-hydroxy-tetrazepam and nortetrazepam.[41][42] The pharmacological effects of tetrazepam are significantly less potent when compared against diazepam, in animal studies.[43] Tetrazepam is a benzodiazepine site agonist and binds unselectively to type 1 and type 2 benzodiazepine site types as well as to peripheral benzodiazepine receptors.[44] The muscle relaxant properties of tetrazepam are most likely due to a reduction of calcium influx.[45] Small amounts of diazepam as well as the active metabolites of diazepam are produced from metabolism of tetrazepam.[46][47] The metabolism of tetrazepam has led to false accusations of prisoners prescribed tetrazepam of taking illicit diazepam; this can lead to increased prison sentences for prisoners.[41]

Abuse

Tetrazepam as with other benzodiazepines is sometimes abused. It is sometimes abused to incapacitate a victim in order to carry out a drug-facilitated crime.[48] or abused in order to achieve a state of intoxication.[49] Tetrazepam's abuse for to carry out drug facilitated crimes may be less however, than other benzodiazepines due to its reduced hypnotic properties.[50]

See also

References

  1. NL Patent 6600095
  2. Recommendation to suspend tetrazepam-containing medicines endorsed by CMDh, European Medicines Agency, published 29 April 2013
  3. Ruhen der Zuhlassung aller Tetrazepam-haltiger Arzneimittel, Sanofi-Avensis Deutschland GmbH (German), published June 2013
  4. 4.0 4.1 "Acute generalized exanthematous pustulosis due to tetrazepam". Journal of Investigational Allergology & Clinical Immunology 18 (2): 119–22. 2008. PMID 18447141. http://www.jiaci.org/issues/vol18issue2/7.pdf. 
  5. "Comparative study in mice of tetrazepam and other centrally active skeletal muscle relaxants". Archives Internationales de Pharmacodynamie et de Therapie 297: 272–85. January 1989. PMID 2567153. 
  6. "Relaxant effect of tetrazepam on rat uterine smooth muscle: role of calcium movement". The Journal of Pharmacy and Pharmacology 48 (11): 1169–73. November 1996. doi:10.1111/j.2042-7158.1996.tb03915.x. PMID 8961167. 
  7. "Benzodiazepine Names". non-benzodiazepines.org.uk. http://www.non-benzodiazepines.org.uk/benzodiazepine-names.html. 
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  9. "Tetrazepam allergy once more detected by patch test". Contact Dermatitis 26 (4): 281. April 1992. doi:10.1111/j.1600-0536.1992.tb00259.x. PMID 1356710. 
  10. "Tetrazepam: an allergen with several clinical expressions". Contact Dermatitis 33 (1): 63–5. July 1995. doi:10.1111/j.1600-0536.1995.tb00462.x. PMID 7493477. 
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  13. "Probable drug rash with eosinophilia and systemic symptoms syndrome related to tetrazepam". Journal of the European Academy of Dermatology and Venereology 22 (7): 887–9. July 2008. doi:10.1111/j.1468-3083.2007.02490.x. PMID 18031497. 
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  18. "Toxic epidermal necrolysis caused by tetrazepam". International Journal of Dermatology 45 (10): 1260–1. October 2006. doi:10.1111/j.1365-4632.2006.03061.x. PMID 17040464. 
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  26. 26.0 26.1 26.2 "Erythema multiforme to tetrazepam". Journal of Investigational Allergology & Clinical Immunology 17 (3): 205–6. 2007. PMID 17583114. http://www.jiaci.org/issues/vol17issue03/14to17.pdf. 
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  40. "Benzodiazepine dependence: focus on withdrawal syndrome". Annales Pharmaceutiques Françaises 67 (6): 408–13. November 2009. doi:10.1016/j.pharma.2009.07.001. PMID 19900604. 
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  42. "Biotransformation and pharmacokinetics of tetrazepam in man". Arzneimittel-Forschung 34 (6): 724–9. 1984. PMID 6148954. 
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  44. "Tetrazepam: a benzodiazepine which dissociates sedation from other benzodiazepine activities. II. In vitro and in vivo interactions with benzodiazepine binding sites". The Journal of Pharmacology and Experimental Therapeutics 245 (2): 699–705. May 1988. PMID 2896795. 
  45. "Spasmolytic effects of tetrazepam on rat duodenum and guinea-pig ileum". Pharmacological Research 35 (5): 493–7. May 1997. doi:10.1006/phrs.1997.0173. PMID 9299217. 
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  48. "Windows of detection of tetrazepam in urine, oral fluid, beard, and hair, with a special focus on drug-facilitated crimes". Therapeutic Drug Monitoring 27 (5): 565–70. October 2005. doi:10.1097/01.ftd.0000164610.14808.45. PMID 16175127. 
  49. "Screening and confirmatory method for benzodiazepines and hypnotics in oral fluid by LC-MS/MS". Forensic Science International 150 (2–3): 213–20. June 2005. doi:10.1016/j.forsciint.2004.12.040. PMID 15944062. 
  50. "Detection of diazepam in urine, hair and preserved oral fluid samples with LC-MS-MS after single and repeated administration of Myolastan and Valium". Analytical and Bioanalytical Chemistry 388 (7): 1545–56. August 2007. doi:10.1007/s00216-007-1297-9. PMID 17468852.