A phase 1 study to assess potential interaction between ASP8062 and alcohol in healthy adult subjects

JOURNAL OF PSYCHOPHARMACOLOGY(2022)

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摘要
Background: ASP8062 is a novel orally active GABA(B) receptor positive allosteric modulator in clinical development for the treatment of alcohol use disorder (AUD) and opioid use disorder (OUD). Aims: This study assessed the potential pharmacokinetic/pharmacodynamic interaction between ASP8062 and alcohol under single-dose conditions in healthy adults. Methods: A double-blind, placebo-controlled, crossover phase 1 study was conducted in which 20 subjects were randomly assigned to four treatment sequences (ASP8062 + alcohol; ASP8062 + placebo alcohol; placebo + alcohol; placebo + placebo alcohol) each consisting of four treatment periods, separated by washout periods of at least 14 days. An analysis of variance was used to assess pharmacokinetic interaction and a mixed-effects analysis of covariance was used to assess pharmacodynamic interaction. Results/outcomes: After administration of alcohol, a mild to minimal increase in plasma exposure (AUC(inf) and C-max) of ASP8062 was observed, but t(max) and t(1/2) for ASP8062 remained unchanged after administration of alcohol. In contrast, ASP8062 did not affect the AUC(last) and C-max of ethanol. No clinically relevant differences in cognition measurements were observed with ASP8062 compared with placebo, but there were expected impairments in psychomotor and executive function with alcohol alone. ASP8062 in combination with alcohol resulted in worse scores in cognition measurements than alcohol alone, but this potentiation was not consistent. ASP8062 administered alone was safe and well-tolerated and safety findings in subjects administered alcohol alone were not augmented when ASP8062 was administered in combination with alcohol. Conclusion/interpretation: The data support further clinical studies investigating ASP8062 in patients with AUD.
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关键词
GABA(B)-receptor positive allosteric modulator, safety, tolerability, pharmacokinetics, pharmacodynamics, alcohol interaction
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