Novel Cross-Species Neurophysiological Assays of Reward and Cognitive Domains

奖励和认知领域的新型跨物种神经生理学测定

• 批准号: 9244071
• 负责人: Diego A Pizzagalli
• 金额: $ 73.18万
• 依托单位: MCLEAN HOSPITAL
• 依托单位国家: 美国
• 财政年份: 2016
• 资助国家: 美国
• 起止时间: 2016-04-01 至 2018-06-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/9244071
• 关键词: Address; Amisulpride; Animal Testing; Animals; Anterior; Area; Behavior; Behavior assessment; Behavioral; Behavioral Assay; Biological Assay; Brain; Characteristics; Chronic; Cognition; Cognition Disorders; Cognitive; Cognitive deficits; Collaborations; Computer Simulation; Coupling; Data; Development; Dimensions; Disease; Dopamine; Dorsal; Dose; Electrodes; Electroencephalography; Electrophysiology (science); Enhancers; Evaluation; Event-Related Potentials; Feedback; Foundations; Frequencies; Goals; Human; Impaired cognition; Laboratory Animals; Lateral; Learning; Link; Measures; Modafinil; Modeling; Molecular; Morbidity - disease rate; National Institute of Mental Health; Neurosciences; Nootropic Agents; Performance; Pharmaceutical Preparations; Pharmacology; Phase; Positioning Attribute; Prefrontal Cortex; Rat-1; Rattus; Reaction Time; Recovery of Function; Research; Research Domain Criteria; Reversal Learning; Rewards; Rodent; Serotonin; Solid; Task Performances; Techniques; Testing; Time; base; behavioral construct; cingulate cortex; cognitive control; effective therapy; flexibility; improved; neural circuit; neurobiological mechanism; neurophysiology; neuropsychiatric disorder; neurotransmission; novel; pre-clinical; public health relevance; receptor; relating to nervous system; research and development; response; source localization; temporal measurement; transmission process; virtual

 DESCRIPTION (provided by applicant): Deficits across the domains of reward and cognition are defining characteristics of virtually all neuropsychiatric disorders, and have deleterious effects on functional recovery, disease chronicity, and morbidity. Development of effective treatments is hindered by the lack of well-validated preclinical measures of target engagement that are functionally similar across species. Capitalizing on a partnership among basic and translational neuroscientists with a strong track record of collaborations, the overarching goal of this UH2/UH3 application is to develop new translational assessments of reward and cognition in which the neurophysiological and behavioral metrics are identical across species. We will address this objective by modifying and validating assessments of reward learning, cognitive control, and cognitive flexibility, each of which is disrupted across illnesses. During the UH2 phase, we will modify and test existing human and rodent versions of a probabilistic reward task (PRT; reward learning), a flanker task (cognitive control) [alternative task: 4-choice serial reaction time task], a probabilistic reversal learning task (PRL; cognitive flexibility), such that task parameters are analogous between humans and rats. Additionally, we will record EEG data in both humans and rats during performance of each task. In both species, EEG data will be analyzed using several techniques, including frequency-domain multi-taper power spectral analyses, time-domain event-related potential (ERP) analyses, and cross-frequency phase-amplitude coupling analyses. In humans, distributed source localization analyses will focus on a priori regions, such as the dorsal anterior cingulate cortex (dACC; reward learning and cognitive control), dorsolateral prefrontal cortex (DLPFC; cognitive control), and lateral orbitofrontal cortx (OFC; reversal learning); EEG electrodes in rats will be placed over homologous regions. We hypothesize that by increasing the congruence of task parameters, task-related behavioral and neurophysiological assays will be similar across species. The two tasks that show the highest neurophysiological (and behavioral) concordance between humans and rats will be advanced to the UH3 phase, in which the selected task(s) will be validated with pharmacological challenges. Specifically, reward learning, cognitive control, or reversal learning and their respective neurophysiological mechanisms will be probed after administration of either the dopamine D2/D3 receptor antagonist amisulpride, the serotonin neurotransmission enhancer vortioxetine, or the cognitive enhancer modafinil. Each pharmacological challenge is based on specific a priori hypotheses regarding neurobiological mechanisms underlying each behavioral construct. Ultimately, these studies will provide novel measures of reward and/or cognition in both humans and rats that show clear parallels in behavior and neurophysiology that can be manipulated with putative treatments across species. Such tasks will help narrow the existing translational gap between preclinical animal and human research and will promote the development of urgently needed treatments for reward and cognitive disorders.

 描述（由申请人提供）：奖励和认知领域的缺陷实际上是所有神经精神疾病的特征，并且对功能恢复、疾病慢性化和发病率产生有害影响。由于缺乏良好的治疗方法，有效治疗的发展受到阻碍。利用具有良好合作记录的基础神经科学家和转化神经科学家之间的伙伴关系，对跨物种功能相似的目标参与进行验证的临床前测量。 这个 UH2/UH3 应用程序旨在开发新的奖励和认知转化，其中神经生理学和行为指标在不同物种之间是相同的。我们将通过修改和验证奖励学习、认知控制和认知灵活性的评估来实现这一目标。在 UH2 阶段，我们将修改和测试现有的人类和啮齿动物版本的概率奖励任务（PRT；奖励学习）、侧翼任务（认知控制）[替代任务： 4-选择串行反应时间任务]，概率逆转学习任务（PRL；认知灵活性），使得 此外，我们将在执行每个任务期间记录人类和大鼠的脑电图数据，并使用多种技术对脑电图数据进行分析，包括频域多锥度功率谱分析。 、时域事件相关电位（ERP）分析和跨频相位振幅耦合分析在人类中，分布式源定位分析将集中于先验区域，例如背侧前扣带皮层（dACC；奖励学习）。和认知控制）、背外侧前额皮质（DLPFC；认知控制）和外侧眶额皮质（OFC；逆转学习）；我们将大鼠的脑电图电极放置在同源区域上，以提高任务参数的一致性。显示人类和大鼠之间最高神经生理学（和行为）一致性的两项任务将进入 UH3 阶段，即跨物种的行为和神经生理学检测。所选择的任务将通过药理学挑战进行验证，特别是奖励学习、认知控制或逆转学习，并且在施用多巴胺 D2/D3 受体拮抗剂氨磺必利、血清素神经传递增强剂沃替西汀后将探讨它们各自的神经生理学机制。 ，或认知增强剂莫达非尼。每个药理学挑战都是基于关于每个行为结构背后的神经生物学机制的特定先验假设，最终，这些研究将提供新的措施。人类和大鼠的奖励和/或认知在行为和神经生理学方面表现出明显的相似性，可以通过跨物种的假定治疗来操纵这些任务将有助于缩小临床前动物和人类研究之间现有的转化差距，并将促进临床前研究的发展。奖励和认知障碍急需治疗。