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关于在精神分裂症中基于神经可塑性的听觉学习的D-丝氨酸增强作用的资助报告。

Grant Report on d-Serine Augmentation of Neuroplasticity-Based Auditory Learning in Schizophrenia .

作者信息

de la Garrigue Natalie, Glasser Juliana, Sehatpour Pejman, Iosifescu Dan V, Dias Elisa, Carlson Marlene, Shope Constance, Sobeih Tarek, Choo Tse-Hwei, Wall Melanie M, Kegeles Lawrence S, Gangwisch James, Mayer Megan, Brazis Stephanie, De Baun Heloise M, Wolfer Stephanie, Bermudez Dalton, Arnold Molly, Rette Danielle, Meftah Amir M, Conant Melissa, Lieberman Jeffrey A, Kantrowitz Joshua T

机构信息

New York State Psychiatric Institute, New York, NY 10032, USA.

Columbia University, College of Physicians and Surgeons, New York, NY 10032, USA.

出版信息

J Psychiatr Brain Sci. 2020;5(4). Epub 2020 Aug 6.

Abstract

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 -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".

摘要

我们报告了一项正在进行的由美国国立精神卫生研究所(NIMH)资助的针对精神分裂症/分裂情感性障碍的R61 - R33项目的基本原理和设计。该项目研究用D - 丝氨酸增强听觉神经可塑性认知康复(AudRem)的疗效,D - 丝氨酸是一种N - 甲基 - D - 天冬氨酸型谷氨酸受体(NMDAR)甘氨酸位点激动剂。我们将AudRem后连续听觉刺激之间音高(频率)的改善(更低)阈值作为可塑性改善的指标,并将失配负波(MMN)和听觉θ波作为NMDAR激动作用和可塑性功能靶点参与的测量指标。先前的研究表明,单独的AudRem能产生显著但较小的认知改善,而单独的D - 丝氨酸能改善症状和MMN。然而,当将D - 丝氨酸和AudRem联合使用时,发现可塑性结果(改善的音高阈值、听觉MMN和θ波)最为显著。AudRem的改善与阅读及其他听觉认知任务相关,表明可塑性的改善可预测功能相关结果。虽然D - 丝氨酸似乎对急性增强AudRem有效,但最佳剂量仍是一个悬而未决的问题,联合使用D - 丝氨酸 + AudRem能否产生持续改善也是如此。在正在进行的R61阶段,45名精神分裂症患者将被随机分配,在三个独立的每组15名受试者的剂量队列(80/100/120 mg/kg)中接受三次安慰剂对照、双盲的D - 丝氨酸 + AudRem治疗。R61阶段的成功完成定义为目标参与度有≥中度的效应量变化且与功能相关,且无安全问题。在为期三年的R33阶段,我们将评估D - 丝氨酸 + AudRem的持续效果。除了测试一种可能可行的治疗方法外,该项目还将开发一种方法,以D - 丝氨酸作为“金标准”来评估新型NMDAR调节剂的疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a52/7448686/7573f650a542/nihms-1619351-f0001.jpg

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