, 5 mg capsules, are sometimes used as an alternative to
diazepam for benzodiazepine withdrawal. Like diazepam, it has a long
elimination half-life and long-acting
active metabolites. Management of benzodiazepine dependence involves considering the person's
age,
comorbidity and the
pharmacological pathways of benzodiazepines. Psychological interventions may provide a small but significant additional benefit over gradual dose reduction alone at post-cessation and at follow-up. With sufficient motivation and the proper approach, almost anyone can successfully withdraw from benzodiazepines. However, a prolonged and severe withdrawal syndrome can cause profound disability, which may lead to breakdown of relationships, loss of employment, financial difficulties, as well as more serious adverse effects such as hospitalization and suicide. As such, long-term users should not be forced to discontinue against their will.
Medications While some substitutive pharmacotherapies may have promise, current evidence is insufficient to support their use. Some studies found that the abrupt substitution of substitutive pharmacotherapy was actually less effective than gradual dose reduction alone, and only three studies found benefits of adding
melatonin,
paroxetine,
trazodone, in conjunction with a gradual dose reduction. Antipsychotics should be avoided during benzodiazepine withdrawal as they tend to aggravate withdrawal symptoms, including convulsions. Some
antipsychotic agents may be riskier than others during withdrawal, especially
clozapine,
olanzapine or low potency
phenothiazines (e.g.,
chlorpromazine), as they lower the
seizure threshold and can worsen withdrawal effects; if used, extreme caution is required. •
Barbiturates are
cross tolerant to benzodiazepines and should generally be avoided; however
phenobarbital can be used, as it is relatively safe, see below. •
Benzodiazepines or
cross tolerant drugs should be avoided after discontinuation, even occasionally. These include the
nonbenzodiazepines
Z-drugs, which have a similar mechanism of action. This is because tolerance to benzodiazepines has been demonstrated to be still present at four months to two years after withdrawal depending on personal biochemistry. Re-exposures to benzodiazepines typically resulted in a reactivation of the tolerance and benzodiazepine withdrawal syndrome. •
Bupropion, which is used primarily as an
antidepressant and smoking cessation aid, is contraindicated in people experiencing abrupt withdrawal from benzodiazepines or other
sedative-hypnotics (e.g. alcohol), due to an increased risk of seizures. •
Buspirone augmentation was not found to increase the discontinuation success rate. •
Caffeine may worsen withdrawal symptoms because of its stimulatory properties. •
Carbamazepine, an
anticonvulsant, appears to have some beneficial effects in the treatment and management of benzodiazepine withdrawal; however, research is limited and thus the ability of experts to make recommendations on its use for benzodiazepine withdrawal is not possible at present. •
Flumazenil has been found to stimulate the reversal of tolerance and the normalization of receptor function. However, further research is needed in the form of randomised trials to demonstrate its role in the treatment of benzodiazepine withdrawal. Flumazenil stimulates the up-regulation and reverses the
uncoupling of
benzodiazepine receptors to the
GABAA receptor, thereby reversing tolerance and reducing withdrawal symptoms and relapse rates. Because of limited research and experience compared to the possible risks involved, the flumazenil detoxification method is controversial and can only be done as an inpatient procedure under medical supervision. :Flumazenil was found to be more effective than placebo in reducing feelings of hostility and aggression in patients who had been free of benzodiazepines for 4–266 weeks. This may suggest a role for flumazenil in treating protracted benzodiazepine withdrawal symptoms. :A study into the effects of the benzodiazepine receptor antagonist, flumazenil, on benzodiazepine withdrawal symptoms persisting after withdrawal was carried out by Lader and Morton. Study subjects had been benzodiazepine-free for between one month and five years, but all reported persisting withdrawal effects to varying degrees. Persistent symptoms included clouded thinking, tiredness, muscular symptoms such as neck tension,
depersonalisation,
cramps and
shaking and the characteristic
perceptual symptoms of benzodiazepine withdrawal, namely, pins and needles feeling, burning skin, pain and subjective sensations of bodily distortion. Therapy with 0.2–2 mg of flumazenil
intravenously was found to decrease these symptoms in a
placebo-controlled study. This is of interest as benzodiazepine receptor antagonists are neutral and have no clinical effects. The author of the study suggested the most likely explanation is past benzodiazepine use and subsequent tolerance had locked the conformation of the GABA-BZD receptor complex into an
inverse agonist conformation, and the
antagonist flumazenil resets benzodiazepine receptors to their original sensitivity. Flumazenil was found in this study to be a successful treatment for protracted benzodiazepine withdrawal syndrome, but further research is required. A study by Professor Borg in Sweden produced similar results in patients in protracted withdrawal. In 2007,
Hoffmann–La Roche the makers of flumazenil, acknowledged the existence of protracted benzodiazepine withdrawal syndromes, but did not recommended flumazenil to treat the condition. •
Fluoroquinolone antibiotics have been noted to increase the incidence of a CNS toxicity from 1% in the general population, to 4% in benzodiazepine-dependent population or in those undergoing withdrawal from them. This is probably the result of their GABA antagonistic effects as they have been found to competitively displace benzodiazepines from benzodiazepine receptor sites. This antagonism can precipitate acute withdrawal symptoms, that can persist for weeks or months before subsiding. The symptoms include depression, anxiety, psychosis,
paranoia, severe
insomnia,
paresthesia,
tinnitus, hypersensitivity to light (
photophobia) and sound (
hyperacusis),
tremors,
status epilepticus, suicidal thoughts and suicide attempt. Fluoroquinolone antibiotics should be contraindicated in patients who are dependent on or in benzodiazepine withdrawal.
NSAIDs have some mild GABA antagonistic properties and animal research indicate that some may even displace benzodiazepines from their binding site. However, NSAIDs taken in combination with fluoroquinolones cause a very significant increase in GABA antagonism, GABA toxicity, seizures, and other severe adverse effects. •
Imidazenil has received some research for management of benzodiazepine withdrawal, but is not currently used in withdrawal. •
Imipramine was found to statistically increase the discontinuation success rate. •
Pregabalin may help reduce the severity of benzodiazepine withdrawal symptoms, and reduce the risk of relapse. •
Propranolol was not found to increase the discontinuation success rate. •
Trazodone was not found to increase the discontinuation success rate.
Inpatient treatment Inpatient drug detox or rehabilitation facilities may be inappropriate for those who have become tolerant or dependent while taking the drug as prescribed, as opposed to recreational use. Such inpatient referrals may be traumatic for these individuals. ==Prognosis==