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C. Strote

HMNC Brain Health

2 papers in the library · publishing 2024-2025

Papers

Antidepressant effect of ketamine unrelated to dissociation: Results from an exploratory mediation analysis of the KET01-02 study

European Psychiatry April 1, 2025 L. Arvastson, E. Papanastasiou, K. Schmid et al.

A novel oral prolonged-release ketamine formulation (KET01) produces lower and delayed peak ketamine concentrations and higher levels of its metabolites, with limited dissociative effects compared to other ketamine formulations. In a randomized, double-blind phase 2 trial, 122 outpatients with treatment-resistant depression received 120 mg, 240 mg, or placebo daily for three weeks. A mediation analysis showed that the antidepressant effect of KET01 was not significantly mediated through dissociation, with an estimated mediation of -1.28% (confidence interval -28% to +11%). This challenges the common view that dissociation is necessary for ketamine's antidepressant effect, suggesting dissociative symptoms are merely adverse events of certain formulations.

Rapid reduction of depressive symptoms with minimal dissociation: results from the KET01-02 and KET01-03 trials with oral prolonged-release (PR) ketamine KET01

European Psychiatry April 1, 2024 C. Zu Eulenburg, E. Papanastasiou, K. Schmid et al.

A novel oral prolonged-release ketamine formulation (KET01) produces a low and delayed peak concentration of ketamine, high hydroxynorketamine levels, and minimal dissociative effects. In a phase 2 trial in outpatients with treatment-resistant depression, 240 mg/day KET01 added to ongoing treatment reduced depressive symptoms within 7 hours, with a statistically significant separation from placebo on day 4 and day 7, though the difference was not significant at day 21. In a separate phase 1 trial in healthy volunteers, the mean maximum dissociative score was 0.7 for KET01 versus 29.6 for intranasal esketamine. The formulation appears to be a safe, take-at-home adjunct treatment with minimal dissociation.