GABAergic modulation of secondary hyperalgesia: A randomized controlled 4-way crossover trial with the α2-subunit preferring GABA positive allosteric modulator, N-desmethyl-clobazam in healthy volunteers

Alain Matthey; Youssef Daali; François Curtin; Antoine Poncet; Jules Desmeules; Marie Besson

doi:10.1002/ejp.1554

GABAergic modulation of secondary hyperalgesia: A randomized controlled 4-way crossover trial with the α2-subunit preferring GABA positive allosteric modulator, N-desmethyl-clobazam in healthy volunteers

Eur J Pain. 2020 Jul;24(6):1094-1106. doi: 10.1002/ejp.1554. Epub 2020 Apr 1.

Authors

Alain Matthey¹, Youssef Daali^{1

2}, François Curtin^{1

2}, Antoine Poncet³, Jules Desmeules^{1

2}, Marie Besson^{1

2}

Affiliations

¹ Division of Clinical Pharmacology and Toxicology, Multidisciplinary Pain Center, Geneva University Hospitals, Geneva, Switzerland.
² Faculty of Medicine, Geneva University, Geneva, Switzerland.
³ Division of Clinical Epidemiology, Geneva University Hospitals, Geneva, Switzerland.

PMID: 32171038
DOI: 10.1002/ejp.1554

Abstract

The antihyperalgesic and sedative effects of the α2-subunit preferring GABA_A positive allosteric modulator (GAM), N-desmethyl-clobazam (NDMC), 20 and 60 mg, were assessed in a randomized, placebo and active-controlled (clonazepam 1,5 mg), 4-way crossover study, in healthy volunteers, using the ultraviolet B-induced experimental pain model. Single (20, 40, 60 mg) and repeated doses (20 mg over 15 days) of NDMC pharmacokinetics were evaluated. Thirty-two subjects participated in the study. Primary outcome parameter was maximal change in the area of cutaneous UVB irradiation-induced secondary hyperalgesia (ASH). ASH decreased under all treatments. Mean (SD) relative change was 79 (22)%, 83 (24)%, 77 (30)% and 92 (16)% for placebo, NDMC20, NDMC60 and clonazepam, respectively. Neither absolute change nor relative change in ASH was significantly different between NDMC60 and placebo (mean difference = 2.3 cm² [95% CI 4.0-8.5], p = .462 and 0.4% [-11.9 to 12.6], p = .952, respectively). An overall treatment effect was found on level of sedation. Compared to placebo, sedation was higher under clonazepam (mean difference = 39 mm [30-49] on a visual analogue scale, p < .001) while NDMC was free of sedative effect. NDMC pharmacokinetics after single doses showed poor absorption, but was linear. Steady-state plasma concentrations of NDMC20 were attained within 14 days, with low between-subjects variability. Mean steady-state concentration (C_S-S , SD) reached 209 (22) ng/ml. NDMC absence of sedative effect and its overall well-characterized safety coming from years of utilization as a metabolite from clobazam, raise the prospect of dose escalating trials in patients to quantify its clinical utility. SIGNIFICANCE: This article, presenting the Phase I data of the new antihyperalgesic compound, α2-subunit GABA_A positive allosteric modulator, N-desmethyl-clobazam (NDMC) is exploring the modulation of a new target in the treatment of neuropathic pain. Based on these results and on its preclinical properties NDMC would qualify as a good tool compound to seek confirmation of the clinical utility of selective GABA allosteric modulators in neuropathic pain patients.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Benzodiazepines* / therapeutic use
Clobazam* / therapeutic use
Cross-Over Studies
Double-Blind Method
Healthy Volunteers
Humans
Hyperalgesia* / chemically induced
Hyperalgesia* / drug therapy
gamma-Aminobutyric Acid

Substances

Benzodiazepines
Clobazam
gamma-Aminobutyric Acid

Grants and funding

SPUM33CM30_124117/1/SNSF_/Swiss National Science Foundation/Switzerland