WHO Drug Information Vol. 17, No. 1, 2003: Safety Issues: Tramadol

WHO Drug Information Vol. 17, No. 1, 2003
(2003; 77 pages)

Table of Contents

Reports on Individual Drugs
	Women's Health Initiative Study
	Menopausal combined hormone therapy update: Canada
	Women's Health Initiative data review: USA
	Future of hormone replacement therapy: Australia
	Hormone replacement therapy recommendations: New Zealand
Vaccines and Biomedicines
	Quality assurance and safety of biologicals
		Production and quality control recommendations
		Vaccines
		Blood products
		International Reference Materials
Current Topics
	Direct-to-consumer drug advertising: survey results
	Race and ethnicity data in clinical trials
	HIV vaccine update
	Drug bar code regulation proposed
	Terminology in pharmacogenetics
	New tool to boost access to quality medicines and detect counterfeits
Safety Issues
	WHO Drug Dictionary: new structure - new focus
	Tramadol - safety experience
	Minocycline and intracranial hypertension
	Neuropsychiatric events: celecoxib and rofecoxib
	Linezolid: peripheral neuropathy
	Zonisamide and visual hallucinations
	Salmeterol study halted
	Labelling and manufacturing of dietary supplements
	Dietary supplements containing ephedra
	Topical use of Lindane
Essential Medicines
	Use of praziquantel in pregnant and lactating women
	Benzimidazoles: use in children
	Praziquantel 'dose pole' for large scale deworming
	Poor access to praziquantel at the peripheral health care level
Regulatory and Safety Action
	New class of HIV treatment approved
	Influenza vaccine composition: Northern hemisphere
	New labelling for conjugated estrogens
	Fibrinolytics in diabetic patients
	Precautions for blood and urine-derived products
	Gefitinib: safety measures
	Nefazodone: marketing suspended
	Amifostine: serious reactions
	Sirolimus: not recommended in lung transplant
	Interferon beta-1a: strengthened labelling
	Palivizumab: prescribing information changes
	Epigallocatechin gallate marketing suspension
	Pergolide mesilate: strengthened warning
Recent Publications and Sources of Information
	WHO's new bookshop
	WHO monographs on medicinal plants
	International Pharmacopoeia: Volume 5
	HIV treatment newsletter
	Malaria: interactive self-assessment
Proposed International Nonproprietary Names: List 88
Annex 1 - PROCEDURE FOR THE SELECTION OF RECOMMENDED INTERNATIONAL NONPROPRIETARY NAMES FOR PHARMACEUTICAL SUBSTANCES*
Annex 2 - GENERAL PRINCIPLES FOR GUIDANCE IN DEVISING INTERNATIONAL NONPROPRIETARY NAMES FOR PHARMACEUTICAL SUBSTANCES*
Annexe 1 - PROCEDURE A SUIVRE EN VUE DU CHOIX DE DENOMINATIONS COMMUNES INTERNATIONALES RECOMMANDEES POUR LES SUBSTANCES PHARMACEUTIQUES
Annexe 2 - DIRECTIVES GENERALES POUR LA FORMATION DE DENOMINATIONS COMMUNES INTERNATIONALES APPLICABLES AUX SUBSTANCES PHARMACEUTIQUES*
Anexo 1 - PROCEDIMIENTO DE SELECCION DE DENOMINACIONES COMUNES INTERNACIONALES RECOMENDADAS PARA LAS SUSTANCIAS FARMACEUTICAS
Anexo 2 - PRINCIPIOS GENERALES DE ORIENTACION PARA FORMAR DENOMINACIONES COMUNES INTERNACIONALES PARA SUSTANCIAS FARMACEUTICAS*

Tramadol - safety experience

Tramadol (Tramal®) is a centrally acting analgesic which has been available in Australia for four years. Although chemically unrelated to the opiates, it stimulates opioid receptors and inhibits noradrenaline and serotonin uptake.

The Australian Adverse Drug Reactions Committee (ADRAC) has received 354 reports associated with tramadol. The most common reactions include nausea, vomiting, sweating, dizziness, rash, tremor and headache. The more serious adverse reactions reported are:

Reaction	No. of reports
Confusion	36
Hallucinations	30
Convulsions	26
Serotonin syndrome	20
Increase in blood pressure	14
Hypersensitivity reactions	12
Hepatic reactions	10
Warfarin interaction	5

For the cases of convulsions, the median time to onset was 2 (range 1-19) days. Tramadol was the only suspected drug in 11 cases, but in 14 other cases the patient was taking additional drugs which may lower the seizure threshold, including propofol, bupropion, hydrocortisone, morphine, and tricyclic antidepressants. One patient had a history of epilepsy, and was also taking carbamazepine and phenytoin.

Tramadol may cause serotonin syndrome, particularly when it is used at high doses or in combination with other agents increasing serotonin levels (1). In 16 of the 20 cases, the patient was taking potentially interacting medicines including moclobemide, SSRIs, tricyclic antidepressants, sibutramine and St John's wort. Increases in hepatic enzymes were reported in 10 cases. One patient developed hepatic failure and died. All times to onset were short (range 1-19 days; median 9 days).

Tramadol may interact with warfarin to decrease prothrombin activity, although the mechanism is unknown (2). ADRAC has received five reports of this interaction. Monitoring should be considered when tramadol is started in patients taking warfarin. Although tramadol acts on opioid receptors, dependence and abuse appear to be rare (3). ADRAC has, however, received 11 reports of withdrawal symptoms with tramadol.

The use of tramadol has increased rapidly, with dispensings of oral formulations rising from 23 000 in 2000 to 580 000 in 2001 and over 1 100 000 in 2002. Prescribers should be alert to the more serious adverse reactions, especially those of a neuropsychiatric nature (4).

References

1. ADRAC. Tramadol and serotonin syndrome. Australian Adverse Drug Reactions Bulletin, 21: 14 (2001).

2. Sabbe, J.R., Sims, P.J., Sims, M.H. Tramadol-warfarin interaction. Pharmacotherapy, 18: 871-873 (1998).

3. FDA Committee. FDC ('Pink Sheets') Prescription Pharmaceuticals and Biotechnology, 60(18): 4-5 (1998).

4. ADRAC. Tramadol - Four years' experience. Australian Adverse Drug Reactions Bulletin, 22(1): 2 (2003).