A comparison of the concentration‐effect relationships of midazolam for EEG‐derived parameters and saccadic peak velocity.

Steveninck, AL Van; Mandema, J.W.; Tuk, B.; Dijk, J.J.M. van; Schoemaker, Rik C.; Danhof, Meindert; Cohen, A. F.

doi:10.1111/j.1365-2125.1993.tb04205.x

Cited by 26 publications

(21 citation statements)

References 15 publications

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“…As expected in most individuals in both groups, there was a strong, significant correlation between EEG beta1 power and plasma midazolam levels supporting previous studies (e.g. Van Steveninck et al 1993). There was no significant difference between the two groups in terms of these correlations.…”

Section: Relationship Between Pharmacokinetic and Pharmacodynamic Measupporting

confidence: 86%

GABA-benzodiazepine receptor function in alcohol dependence: a combined 11C-flumazenil PET and pharmacodynamic study

et al. 2005

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In summary, our study suggests that alcohol dependence in man is associated with a reduced EEG sleep response to the benzodiazepine agonist, midazolam, which is not explained by reduced BDZ receptor occupancy, and is consistent with reduced sensitivity in this measure of GABA-BDZ receptor function in alcohol dependence. The lack of change in other functional measures may reflect a differential involvement of particular subtypes of the GABA-BDZ receptor.

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Section: Relationship Between Pharmacokinetic and Pharmacodynamic Measupporting

confidence: 86%

GABA-benzodiazepine receptor function in alcohol dependence: a combined 11C-flumazenil PET and pharmacodynamic study

et al. 2005

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“…Saccadic peak velocity is one of the most sensitive parameters for sedation and was described previously (Van Steveninck et al, 1991, 1993. Recording and analysis of saccadic eye movements was conducted with a microcomputer-based system for sampling and analysis of eye movements.…”

Section: Saccadic Eye Movementsmentioning

confidence: 99%

No evidence of potentiation of buprenorphine by milnacipran in healthy subjects using a nociceptive test battery

Okkerse

Álvarez-Jiménez

Hay

et al. 2016

European Journal of Pain

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Buprenorphine is known to be a potent opioid agonist. Animal studies suggest that milnacipran co-administered with opioids may potentiate the analgesic effect of μ-opioid receptor agonists. Here, we found that buprenorphine showed a dose-dependent analgesic effect, but that no potentiation or synergy on a battery of evoked pain tasks could be observed after co-administration of both milnacipran and buprenorphine.

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“…The computer‐based measurement of saccadic eye movements was described originally by Baloh . It has been shown to be a sensitive measurement of sedative effects of drugs . Saccadic eye movements were assessed with Compumedics Neuroscan Grael or NuAmp Electroencephalogram amplifiers and Compumedics Curry 7 or Scan 4.5 acquisition and analysis software, respectively.…”

Section: Methodsmentioning

confidence: 99%

First‐in‐man study of ACT‐709478, a novel selective triple T‐type calcium channel blocker

Richard

Kaufmann

Kornberger³

et al. 2019

Epilepsia

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Summary Objective Increased activity of T‐type Ca2+ channels is linked to idiopathic generalized epilepsies, thus blocking these channels may be a new treatment option. ACT‐709478 is an orally available triple T‐type Ca2+ channel blocker. The aim of this first‐in‐man study was to investigate the pharmacokinetics, pharmacodynamics, tolerability, and safety of single doses of ACT‐709478 in healthy subjects. Methods This double‐blind, placebo‐controlled, randomized study included 65 healthy male subjects. Ascending single oral doses of 1‐400 mg ACT‐709478 or placebo were administered to sequential groups of eight subjects (6 on active, 2 on placebo). Effect of food was tested in a crossover part at 60 mg. Blood and saliva sampling for pharmacokinetic evaluations and safety assessments was performed regularly. Effects on the central nervous system were assessed with a battery of pharmacodynamic tests. Results The maximum plasma concentration (Cmax) was reached within 3 to 4 hours (≤60 mg) and within 20 to 28 hours (>60 mg), and across all dose levels the terminal half‐life (95% confidence interval) ranged from 36 (29‐45) to 43 (22‐86) hours. Multiple peaks were observed and Cmax and area under the plasma concentration‐time curve (AUC)0‐∞ increased in a less than dose‐proportional manner. A 1.6‐fold increase in Cmax and no change in AUC0‐∞ was observed in fed compared to fasted conditions. A significant correlation (P < 0.0001) between plasma and saliva concentrations was established using linear regression. All adverse events were transient and of mild or moderate intensity. No treatment‐related effects on vital signs, clinical laboratory, telemetry, or electrocardiography were detected. The results of pharmacodynamic tests did not show relevant mean changes compared to baseline or placebo. Significance ACT‐709478 exhibits good tolerability and safety after single‐dose administration and its pharmacokinetic and pharmacodynamic properties warrant further investigations.

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A comparison of the concentration‐effect relationships of midazolam for EEG‐derived parameters and saccadic peak velocity.

Cited by 26 publications

References 15 publications

GABA-benzodiazepine receptor function in alcohol dependence: a combined 11C-flumazenil PET and pharmacodynamic study

GABA-benzodiazepine receptor function in alcohol dependence: a combined 11C-flumazenil PET and pharmacodynamic study

No evidence of potentiation of buprenorphine by milnacipran in healthy subjects using a nociceptive test battery

First‐in‐man study of ACT‐709478, a novel selective triple T‐type calcium channel blocker

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