Flumazenil in benzodiazepine overdose

Howard An; Jesse Godwin

doi:10.1503/cmaj.160357

Isolated benzodiazepine overdoses are rarely fatal

A population-based retrospective study reported a rate of 3.0–7.9 deaths per million benzodiazepine prescriptions.1 Sedation is common, but severe respiratory depression and hemodynamic instability are rare.2 Supportive care is generally sufficient for the management of benzodiazepine overdose.

Flumazenil antagonizes benzodiazepine activity

Benzodiazepines promote the binding of γ-aminobutyric acid (GABA) to its receptor. The “Z” drugs (zopiclone, zaleplon and zolpidem) act in a similar manner. Flumazenil is a benzodiazepine analogue with minimal intrinsic activity.3 It binds to the extracellular surface of GABA_A receptors and competitively displaces benzodiazepine molecules, preventing further benzodiazepine binding.3

Flumazenil should not be used routinely

Flumazenil is contraindicated in patients with unknown or mixed overdose, benzodiazepine tolerance, seizure disorders or a prolonged QRS interval.3 In a recent meta-analysis, serious adverse events were significantly more common among patients with suspected benzodiazepine overdose treated with flumazenil than among those in the placebo group (risk ratio 3.81, 95% confidence interval 1.28–11.39; number needed to harm = 50).2 Seizures and ventricular dysrhythmias can develop, especially if withdrawal is precipitated in benzodiazepine-tolerant individuals or if flumazenil reverses the protective effect of benzodiazepines in patients with unknown or mixed overdose. 3 Seizures may become more difficult to manage and may require the use of propofol or barbiturates. A poison centre should be consulted if the use of flumazenil is being considered.

Select patients may benefit from the administration of flumazenil

Flumazenil can reverse respiratory depression in the rare patient with severe, isolated benzodiazepine or “Z” drug toxicity who does not have contraindications to its use. It is most often considered in accidental pediatric ingestions or reversal of iatrogenic oversedation. Case reports have shown successful flumazenil reversal of paradoxic reactions (agitation) associated with benzodiazepines.4 Flumazenil does not reverse sedation due to barbiturates, ethanol or opioids.

Flumazenil has a short half-life

Evidence regarding optimal dosing is limited. The manufacturer recommends an initial dose of 0.2 mg given over 15 seconds.5 A suggested, more cautious approach would be to administer flumazenil in 0.1-mg doses (or 0.01 mg/kg) each over one minute, to a maximum of 1 mg, or until an effect is achieved or toxicity develops. 2 The half-life of flumazenil is about 50 minutes, which is shorter than that of most benzodiazepines. Therefore, sedation often recurs. Cardiorespiratory monitoring is necessary, and repeat dosing or infusion may be required.5

Footnotes

Competing interests: None declared. This article has been peer reviewed.

References

↵
1. Buckley NA,
2. McManus PR
. Changes in fatalities due to overdose of anxiolytic and sedative drugs in the UK (1983–1999). Drug Saf 2004;27:135–41.
OpenUrl CrossRef PubMed
↵
1. Penninga EI,
2. Graudal N,
3. Ladekarl MB,
4. et al
. Adverse events associated with flumazenil treatment for the management of suspected benzodiazepine intoxication: a systematic review with meta-analyses of randomised trials. Basic Clin Pharmacol Toxicol 2016;118:37–44.
OpenUrl
↵
1. Sivilotti MLA
. Flumazenil, naloxone and the ‘coma cocktail’.Br J Clin Pharmacol 2016;81:428–36.
OpenUrl
↵
1. Jackson BF,
2. Beck LA,
3. Losek JD
. Successful flumazenil reversal of paradoxical reaction to midazolam in a child. J Emerg Med 2015;48:e67–72.
OpenUrl
↵
Anexate [package insert]. Basel (Switzerland): Hoffman–La Roche; 2008.