Bromazolam: Difference between revisions

Bromazolam is a triazolobenzodiazepine first synthesized by Upjohn in 1976 and never developed clinically. It emerged on the research-chemical market around 2016 and, beginning around 2021–2022, became one of the most commonly encountered designer benzodiazepines in North America — notably as an adulterant in the illicit opioid supply alongside fentanyl and, often, xylazine. Pharmacologically and structurally it is the bromine analog of alprazolam, with comparable potency and a similar (or somewhat longer) duration of action.

None approved. Has no recognized medical role.

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No therapeutic dosing. Harm-reduction note: because of inconsistent tablet purity and frequent fentanyl co-contamination, any illicit "benzo" tablet should be assumed to potentially contain bromazolam, fentanyl, or both.

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Sedation, anxiolysis, anterograde amnesia, ataxia, slurred speech, disinhibition, prolonged blackouts. At high dose or in combination: severe sedation, respiratory depression, coma. Paradoxical agitation/aggression occasionally reported. Withdrawal mirrors other high-potency benzos: anxiety, insomnia, autonomic hyperactivity, seizures, delirium — and can be life-threatening, often more protracted than alprazolam withdrawal owing to the longer half-life.

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Lipophilic; orally bioavailable; hepatic metabolism (CYP3A4 predominantly) with hydroxylated metabolites. Half-life appears longer than alprazolam, with case reports of detection in blood/urine for days after a single exposure. Standard benzodiazepine immunoassay screens frequently miss bromazolam — confirmatory LC-MS/MS is required for reliable detection. Non-selective positive allosteric modulator at the benzodiazepine site of GABA_A receptors containing α1, α2, α3, or α5 subunits with a γ subunit. Like alprazolam, clinically displays anxiolytic, hypnotic, anticonvulsant, amnestic, and muscle-relaxant effects with significant abuse liability. Respiratory depression at high doses is modest in isolation but markedly synergized by opioids, alcohol, and other CNS depressants — the dominant mechanism of bromazolam-associated mortality.

• Opioids (fentanyl, heroin, methadone, buprenorphine): profound additive respiratory depression — primary mechanism of bromazolam-associated overdose death.
• Alcohol, GHB, barbiturates, gabapentinoids: additive CNS/respiratory depression.
• Xylazine: frequently co-encountered in illicit opioid supply ("tranq dope"); compounds sedation and complicates resuscitation (xylazine is not reversed by naloxone).
• CYP3A4 inhibitors (azoles, macrolides, ritonavir, grapefruit): prolong/intensify effect.
• CYP3A4 inducers (rifampin, carbamazepine, phenytoin, St John's wort): may reduce levels.
• Flumazenil reverses GABA_A effects but is rarely used in mixed-overdose / chronic-benzo contexts due to seizure risk.

  Pregnancy and lactation

Avoid in pregnancy and lactation. Class data extrapolated from clinical benzodiazepines; designer status means no formal safety data. In suspected overdose: airway, respiratory rate, oxygen saturation, mental status. Standard urine benzodiazepine immunoassay is insensitive to bromazolam — request specific LC-MS/MS confirmation. ECG and electrolytes if mixed overdose suspected. Patients should be counseled that illicit "Xanax bars" or designer benzodiazepine tablets are frequently bromazolam and/or fentanyl. Never combine with opioids or alcohol. Withdrawal requires medically supervised taper — do not stop abruptly after sustained use. Carry naloxone if any opioid co-use is plausible (naloxone does not reverse bromazolam itself but reverses concurrent opioid depression).

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Alprazolam, Clonazolam, Flualprazolam, Etizolam, Flumazenil, Fentanyl, Xylazine, Naloxone

• DEA Diversion. Bromazolam. Drug & Chemical Evaluation Section, 2023.
• Papsun DM, et al. Forensic toxicology of bromazolam. J Anal Toxicol 2022.
• CFSRE / NPS Discovery. Bromazolam emergence reports, 2021–2024.
• Health Canada / CCENDU bulletins on designer benzodiazepines in the unregulated medicine supply.