Dose-Dependent Augmentation of Neuroplasticity-Based Auditory Learning in Schizophrenia: A Double-Blind, Placebo-Controlled, Randomized, Target Engagement Clinical Trial of the NMDA Glutamate Receptor Agonist d-serine

安慰剂 谷氨酸受体 NMDA受体 精神分裂症(面向对象编程) 神经可塑性 心理学 兴奋剂 医学 麻醉 内科学 药理学 神经科学 精神科 受体 病理 替代医学
作者
Pejman Sehatpour,Dan V. Iosifescu,Heloise M. De Baun,Constance Shope,Megan Mayer,James E. Gangwisch,Elisa C. Dias,Tarek Sobeih,Tse‐Hwei Choo,Melanie M. Wall,Alice Medalia,Alice M. Saperstein,Lawrence S. Kegeles,Ragy R. Girgis,Marlene Carlson,Joshua T. Kantrowitz
出处
期刊:Biological Psychiatry [Elsevier]
卷期号:94 (2): 164-173 被引量:17
标识
DOI:10.1016/j.biopsych.2023.01.015
摘要

Background Patients with schizophrenia show reduced NMDA glutamate receptor–dependent auditory plasticity, which is rate limiting for auditory cognitive remediation (AudRem). We evaluate the utility of behavioral and neurophysiological pharmacodynamic target engagement biomarkers, using a d-serine+AudRem combination. Methods Forty-five participants with schizophrenia or schizoaffective disorder were randomized to 3 once-weekly AudRem visits + double-blind d-serine (80, 100, or 120 mg/kg) or placebo in 3 dose cohorts of 12 d-serine and 3 placebo-treated participants each. In AudRem, participants indicated which paired tone was higher in pitch. The primary outcome was plasticity improvement, operationalized as change in pitch threshold between AudRem tones [(test tone Hz − reference tone Hz)/reference tone Hz] between the initial plateau pitch threshold (mean of trials 20–30 of treatment visit 1) to pitch threshold at the end of visit(s). Target engagement was assessed by electroencephalography outcomes, including mismatch negativity (pitch primary). Results There was a significant overall treatment effect for plasticity improvement (p = .014). Plasticity improvement was largest within the 80 and 100 mg/kg groups (p < .001, d > 0.67), while 120 mg/kg and placebo-treated participants showed nonsignificant within-group changes. Plasticity improvement was seen after a single treatment and was sustained on subsequent treatments. Target engagement was demonstrated by significantly larger mismatch negativity (p = .049, d = 1.0) for the 100 mg/kg dose versus placebo. Conclusions Our results demonstrate sufficient proof of principle for continued development of both the d-serine+AudRem combination and our target engagement methodology. The ultimate utility is dependent on the results of an ongoing larger, longer study of the combination for clinically relevant outcomes.
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