Flumazenil is a competitive benzodiazepine receptor inhibitor. It is classified as an antidote to benzodiazepines.
Indications
The approved indications for flumazenil are:
– Reversal of conscious sedation and general anesthesia
– Suspected benzodiazepine overdose
The usual dose is 0.2 mg over 15-30 seconds, repeated every minute if needed. The onset of action is 1-2 minutes and the effect lasts for about 1 hour.
Controversy in benzodiazepine overdose
Many providers insist on not using flumazenil in benzodiazepine overdose scenarios due to the risk of precipitating acute benzodiazepine withdrawal and seizures.
This risk was described in case reports in the early 1990’s.
A 39-year-old woman who overdosed on benzodiazepines and tricyclic antidepressants was treated with flumazenil. The patient developed refractory seizures. Lorazepam, phenytoin, and phenobarbital were administered; however, seizures persisted for 4 hours, resulting in rhabdomyolysis, acute renal failure, severe brain damage, and death.
Another set of authors reported the occurrence of a generalized tonic-clonic seizure in a pediatric patient following the administration of flumazenil.
A review of 43 seizures reported with flumazenil identified that almost half of the cases involved co-ingestion of a pro-convulsant agent (such as a tricyclic antidepressant).
In addition to these human case reports, rat and dog data suggest the increased risk of seizure when flumazenil is given.
Is the seizure risk overblown?
In the present decade, some slightly more robust data has been presented suggesting the risk of seizure from flumazenil in benzodiazepine toxicity may be overstated.
A single-center retrospective observational study of 23 adult patients administered flumazenil for known or suspected benzodiazepine overdose in the ED, revealed that no patient experienced a seizure.
A poison center published 10 years of data on flumazenil administration in acutely poisoned adults. Out of 904 patients, there were 13 patients with seizures and 1 death following flumazenil administration. 8 of the 13 patients who seized had also taken pro-convulsant medications.
Given this more recent data, it seems unlikely that flumazenil would be harmful when given to overdose patients, and that patients with pro-convulsant co-ingestion might be the only group to be concerned about.
What is flumazenil good for?
While it may be true that flumazenil is relatively safe, I am not impressed with the benefit that it is likely to offer benzodiazepine overdose patients.
Firstly, in the 10-year study by the poison center, only half of the patients who received flumazenil woke up afterward.
Secondly, flumazenil might not reverse the respiratory depressive effects of benzodiazepines! A 1993 article concluded:
When benzodiazepine-induced respiratory depression was evident, the ability of flumazenil to reverse it was inconsistent and short-lived.
Benzodiazepine toxicity is easily treated with supportive care, so to use an antidote that does not consistently work is not appealing to me, no matter how small the risk of seizure may be. If I am going to use flumazenil in benzodiazepine toxicity, I want there to be a significant diagnostic value. Perhaps avoiding a lumbar puncture or other invasive procedure would make it worthwhile.
Summary
In toxicology scenarios, flumazenil has little to no therapeutic value. Lack of benefit rather than risk of harm is my reason for almost never using flumazenil.