Literature DB >> 1888441

Benzodiazepine poisoning. Clinical and pharmacological considerations and treatment.

P Gaudreault1, J Guay, R L Thivierge, I Verdy.   

Abstract

Benzodiazepines are among the most frequently prescribed drugs worldwide. This popularity is based not only on their efficacy but also on their remarkable safety. Pure benzodiazepine overdoses usually induce a mild to moderate central nervous system depression; deep coma requiring assisted ventilation is rare, and should prompt a search for other toxic substances. The severity of the CNS depression is influenced by the dose, the age of the patient and his or her clinical status prior to the ingestion, and the coingestion of other CNS depressants. In severe overdoses, benzodiazepines can occasionally induce cardiovascular and pulmonary toxicity, but deaths resulting from pure benzodiazepine overdoses are rare. Quantitative determinations of benzodiazepines are not useful in the clinical management of intoxicated patients since there is no correlation between serum concentrations and pharmacological and toxicological effects. Benzodiazepine overdoses occurring during pregnancy rarely induce serious morbidity in mothers or fetuses, although large doses administered near delivery can induce respiratory depression in neonates. The teratogenic potential of benzodiazepines remains controversial, but is probably small if it exists at all. There is clear evidence that the prolonged use of even therapeutic doses of benzodiazepines will lead to dependence. The risk of developing significant withdrawal symptoms is related to dosage and duration of treatment. Prevention of gastrointestinal absorption should be initiated in all intentional benzodiazepine overdoses. Forced diuresis and dialysis techniques are not indicated since they will not significantly accelerate the elimination of these agents. Intravenous administration of flumazenil, a pure benzodiazepine antagonist, effectively reverses benzodiazepine-induced CNS depression.

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Year:  1991        PMID: 1888441     DOI: 10.2165/00002018-199106040-00003

Source DB:  PubMed          Journal:  Drug Saf        ISSN: 0114-5916            Impact factor:   5.606


  225 in total

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Authors:  G Ziegler; L Ludwig; U Klotz
Journal:  Pharmacopsychiatria       Date:  1983-05

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Authors:  U Klotz; I Reimann
Journal:  N Engl J Med       Date:  1980-05-01       Impact factor: 91.245

6.  RO 15-1788 antagonises the central effects of diazepam in man without altering diazepam bioavailability.

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Journal:  Br J Clin Pharmacol       Date:  1982-11       Impact factor: 4.335

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Journal:  J Pharm Sci       Date:  1981-10       Impact factor: 3.534

8.  Lack of relation of oral clefts to diazepam use during pregnancy.

Authors:  L Rosenberg; A A Mitchell; J L Parsells; H Pashayan; C Louik; S Shapiro
Journal:  N Engl J Med       Date:  1983-11-24       Impact factor: 91.245

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Authors:  P Lheureux; R Askenasi
Journal:  Hum Toxicol       Date:  1988-03

10.  Absolute bioavailability of oral and intramuscular diazepam: effects of age and sex.

Authors:  M Divoll; D J Greenblatt; H R Ochs; R I Shader
Journal:  Anesth Analg       Date:  1983-01       Impact factor: 5.108

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  12 in total

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Authors:  J S Lyons; D B Larson; J Hromco
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7.  Relative toxicity of benzodiazepines in overdose.

Authors:  N A Buckley; A H Dawson; I M Whyte; D L O'Connell
Journal:  BMJ       Date:  1995-01-28

8.  Warnings Unheeded:The Risks of Co-Prescribing Opioids and Benzodiazepines.

Authors:  Shanna Babalonis; Sharon L Walsh
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9.  Benzodiazepine prescription and length of hospital stay at a Japanese university hospital.

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10.  A sound sleep.

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