Flubromazolam – A new life-threatening designer benzodiazepine

Łukasik-Głębocka, Magdalena; Sommerfeld, Karina; Tężyk, Artur; Zielińska-Psuja, Barbara; Panieński, Paweł; Żaba, Czesław

doi:10.3109/15563650.2015.1112907

Cited by 91 publications

(56 citation statements)

References 7 publications

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“…Benzodiazepines were misused long before emerging as NPS and a recent report highlighted the increasing illicit availability and misuse of a clinically used benzodiazepine, alprazolam, often purchased from the dark web . The NPS benzodiazepines (referred to in this work as NPS‐benzodiazepines) have already been reported in a number of overdose cases, driving under the influence of drugs (DUID) cases, and hospital admissions . The lack of control over and safety of these NPS‐benzodiazepines is a prevalent issue and it is predicted that it will become an even more worrying trend as their misuse continues to spread.…”

Section: Introductionmentioning

confidence: 99%

Experimental versus theoretical log D_7.4, pK_a and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

Manchester

Maskell

Waters

2018

Drug Testing and Analysis

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The misuse of benzodiazepines as new psychoactive substances is an increasing problem around the world. Basic physicochemical and pharmacokinetic data is required on these substances to interpret and predict their effects upon humans. Experimental log D , pK and plasma protein binding values were determined for 11 benzodiazepines that have recently appeared as new psychoactive substances (3-hydroxyphenazepam, 4'-chlorodiazepam, desalkylflurazepam, deschloroetizolam, diclazepam, etizolam, flubromazepam, flubromazolam, meclonazepam, phenazepam, and pyrazolam) and compared with values generated by various software packages (ACD/I-lab, MarvinSketch, ADMET Predictor and PreADMET). ACD/I-LAB returned the most accurate values for log D and plasma protein binding while ADMET Predictor returned the most accurate values for pK . Large variations in predictive errors were observed between compounds. Experimental values are currently preferable and desirable as they may aid with the future 'training' of predictive models for these new psychoactive substances.

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Section: Introductionmentioning

confidence: 99%

Experimental versus theoretical log D_7.4, pK_a and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

Manchester

Maskell

Waters

2018

Drug Testing and Analysis

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“…[5] Recently, a case of intoxication of flubromazolam indicated that low plasma concentrations around 0.043 mg/L can cause a deep coma with long-lasting central nervous system-depression. [6] According to online drug users' forums, flubromazolam is a drug with high potency and long duration of action (up to 3 d), with reported user's dose ranging from 0.25 mg on blotters up to 16 mg in tablets for users with high self-reported benzodiazepine tolerance. [7,8] In one reported in vitro study using pooled human liver microsomes (pHLM), one mono and one dihydroxylated metabolite of flubromazolam were tentatively identified, however without assigning the site of the monohydroxylation.…”

Section: Flubromazolam Was First Reported In Sweden In 2014 and Inclumentioning

confidence: 99%

In vitro studies on flubromazolam metabolism and detection of its metabolites in authentic forensic samples

Noble

Mardal

Holm

et al. 2017

Drug Testing and Analysis

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Flubromazolam is a triazole benzodiazepine with high potency and long-lasting central nervous system depressant effects; however, limited data about its pharmacokinetics are available. Here, we report in vitro studies of the human flubromazolam metabolism analyzed by liquid chromatography high-resolution mass spectrometry (LC-HRMS). In vitro investigations were carried out in pooled human liver microsomes (pHLM) and recombinant cytochrome P450 (CYP)-enzymes. To confirm those metabolites detected in vitro, authentic samples obtained from two forensic cases were also analyzed by LC-HRMS. Additionally, determination of the unbound fraction of flubromazolam in pHLM and in plasma was performed by equilibrium dialysis with subsequent prediction of its hepatic clearance (CL ) using well-stirred and parallel-tube models. Additional findings obtained by routine screening methods of these forensic cases are also reported. Studies using incubations with nicotinamide adenine dinucleotide phosphate-fortified pHLM with or without uridine 5'-diphosphoglucuronic acid and incubations with CYP-enzymes identified the main metabolic pathway of flubromazolam as hydroxylation on the α- and/or 4-position mediated by CYP3A4 and CYP3A5, with subsequent glucuronidation of the hydroxylated metabolites as well as of the parent drug. Further, α-hydroxy-flubromazolam and its corresponding glucuronide were detected in vivo together with the N-glucuronide of flubromazolam. The predicted CL of flubromazolam using the well-stirred and parallel-tube models were 0.42 and 0.43 mL/min/kg, respectively. Based on the data presented here, flubromazolam is primarily metabolized by CYP3A4/5 with a high protein-binding and a predicted low clearance. Analysis of authentic samples suggested that analytical targets for flubromazolam should be the compound itself and α-hydroxy-flubromazolam. Copyright © 2016 John Wiley & Sons, Ltd.

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“…7,14 Norflurazepam, also named desalkykflurazepam, is the principal active metabolite of flurazepam, 10,17,18 a BZ hypnotic used in the United States since 1970. 6,[28][29][30][31] In cases of overdose, some designer BZs can be detected with adequate sensitivity by immunoassay-based urine drug screening. 10,21 The principal determinants of elimination 10 This scenario is not difficult to envision if a user is not familiar with a particular compound, or ingests an impure mixture of multiple compounds.…”

Section: Designer Benzodiazepines: a Review Of Published Data And Pubmentioning

confidence: 99%

Designer Benzodiazepines: A Review of Published Data and Public Health Significance

Greenblatt

2019

Clinical Pharm in Drug Dev

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Flubromazolam – A new life-threatening designer benzodiazepine

Abstract: Flubromazolam is a new designer drug. Recreational use may be a cause of prolonged, severe intoxication associated with coma, hypotension, and rhabdomyolysis.

Cited by 91 publications

References 7 publications

Experimental versus theoretical log D_7.4, pK_a and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

Experimental versus theoretical log D_7.4, pK_a and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

In vitro studies on flubromazolam metabolism and detection of its metabolites in authentic forensic samples

Designer Benzodiazepines: A Review of Published Data and Public Health Significance

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Flubromazolam – A new life-threatening designer benzodiazepine

Abstract: Flubromazolam is a new designer drug. Recreational use may be a cause of prolonged, severe intoxication associated with coma, hypotension, and rhabdomyolysis.

Cited by 91 publications

References 7 publications

Experimental versus theoretical log D7.4, pKa and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

Experimental versus theoretical log D7.4, pKa and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

In vitro studies on flubromazolam metabolism and detection of its metabolites in authentic forensic samples

Designer Benzodiazepines: A Review of Published Data and Public Health Significance

Contact Info

Product

Resources

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Experimental versus theoretical log D_7.4, pK_a and plasma protein binding values for benzodiazepines appearing as new psychoactive substances

Experimental versus theoretical log D_7.4, pK_a and plasma protein binding values for benzodiazepines appearing as new psychoactive substances