d-丝氨酸增强精神分裂症患者基于神经可塑性的听觉学习的Grant报告†

Natalie de la Garrigue, Juliana Glasser, P. Sehatpour, D. Iosifescu, E. Dias, Marlene Carlson, Constance B. Shope, T. Sobeih, Tse-Hwei Choo, M. Wall, L. Kegeles, James E. Gangwisch, Megan R Mayer, Stephanie Brazis, Heloise M. De Baun, S. Wolfer, D. Bermudez, Molly S. Arnold, Danielle N. Rette, A. Meftah, M. Conant, J. Lieberman, Joshua T. Kantrowitz
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引用次数: 7

摘要

我们报告了NIMH赞助的R61-R33项目在精神分裂症/分裂情感障碍中的原理和设计。该项目研究用N-甲基-d-天冬氨酸型谷氨酸受体(NMDAR)甘氨酸位点激动剂d-丝氨酸增强听觉神经可塑性认知修复(AudRem)的疗效。我们将AudRem后连续听觉刺激之间音高(频率)的改善(较小)阈值作为可塑性的改善,并将错配负性(MMN)和听觉θ作为NMDAR激动性和可塑性的功能靶标参与的测量。先前的研究表明,单独使用AudRem可以产生显著但微小的认知改善,而单独使用d-丝氨酸可以改善症状和MMN。然而,当结合d-丝氨酸和AudRem时,可塑性结果(改善的音高阈值、听觉MMN和θ)最强。AudRem的改善与阅读和其他听觉认知任务相关,表明可塑性的改善可以预测功能相关的结果。虽然d-丝氨酸似乎对急性AudRem增强有效,但最佳剂量仍然是一个悬而未决的问题,d-丝氨酸+AudRem组合产生持续改善的能力也是一个悬而未决。在正在进行的R61中,45名精神分裂症患者将被随机分组,在三个独立的15名受试者剂量组(80/100/120 mg/kg)中接受三次安慰剂对照、双盲d-丝氨酸+AudRem治疗。R61的成功完成是指在没有安全问题的情况下,目标交战和与功能的相关性发生≥中等效果大小的变化。在为期三年的R33期间,我们将评估d-丝氨酸+AudRem的持续作用。除了测试一种潜在可行的治疗方法外,该项目还将开发一种方法来评估新型NMDAR调节剂的疗效,将d-丝氨酸作为“金标准”。
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Grant Report on d-Serine Augmentation of Neuroplasticity-Based Auditory Learning in Schizophrenia †
We report on the rationale and design of an ongoing NIMH sponsored R61-R33 project in schizophrenia/schizoaffective disorder. This project studies augmenting the efficacy of auditory neuroplasticity cognitive remediation (AudRem) with d-serine, an N-methyl-d-aspartate-type glutamate receptor (NMDAR) glycine-site agonist. We operationalize improved (smaller) thresholds in pitch (frequency) between successive auditory stimuli after AudRem as improved plasticity, and mismatch negativity (MMN) and auditory θ as measures of functional target engagement of both NMDAR agonism and plasticity. Previous studies showed that AudRem alone produces significant, but small cognitive improvements, while d-serine alone improves symptoms and MMN. However, the strongest results for plasticity outcomes (improved pitch thresholds, auditory MMN and θ) were found when combining d-serine and AudRem. AudRem improvements correlated with reading and other auditory cognitive tasks, suggesting plasticity improvements are predictive of functionally relevant outcomes. While d-serine appears to be efficacious for acute AudRem enhancement, the optimal dose remains an open question, as does the ability of combined d-serine + AudRem to produce sustained improvement. In the ongoing R61, 45 schizophrenia patients will be randomized to receive three placebo-controlled, double-blind d-serine + AudRem sessions across three separate 15 subject dose cohorts (80/100/120 mg/kg). Successful completion of the R61 is defined by ≥moderate effect size changes in target engagement and correlation with function, without safety issues. During the three-year R33, we will assess the sustained effects of d-serine + AudRem. In addition to testing a potentially viable treatment, this project will develop a methodology to assess the efficacy of novel NMDAR modulators, using d-serine as a “gold-standard”.
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