An FMRI Study of Three Neural Systems Implicated in Obsessive-Compulsive Disorder

与强迫症有关的三个神经系统的 FMRI 研究

• 批准号: 8096946
• 负责人: RACHEL MARSH
• 金额: $ 19.99万
• 依托单位: NEW YORK STATE PSYCHIATRIC INSTITUTE DBA RESEARCH FOUNDATION FOR MENTAL HYGIENE, INC
• 依托单位国家: 美国
• 财政年份: 2011
• 资助国家: 美国
• 起止时间: 2011-08-01 至 2013-07-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8096946
• 关键词: Adolescence; Adult; Affect; Age; Age of Onset; Amygdaloid structure; Animal Experimentation; Animals; Anterior; Area; Automobile Driving; Behavior; Behavioral Paradigm; Biological Markers; Brain; Clinical; Cognitive; Cognitive Therapy; Corpus striatum structure; Data; Dimensions; Dorsal; Environment; Exploratory/Developmental Grant; Fluoxetine; Fostering; Functional Magnetic Resonance Imaging; Functional disorder; Future; Goals; Habits; Hippocampus (Brain); Human; Image; Individual; Informal Social Control; Learning; MRI Scans; Magnetic Resonance Imaging; Measures; Medial; Mediating; Memory; National Institute of Mental Health; Obsession; Obsessive compulsive behavior; Obsessive-Compulsive Disorder; Outcome; Patients; Pattern; Performance; Pharmaceutical Preparations; Prefrontal Cortex; Process; Response to stimulus physiology; Rewards; Risk; Scanning; Selective Serotonin Reuptake Inhibitor; Severities; Specificity; Strategic Planning; Symptoms; System; Temporal Lobe; Testing; Thinking; Time; base; biosignature; cingulate cortex; design; habit learning; innovation; neurochemistry; neuroimaging; neuromechanism; novel; prospective; relating to nervous system; response; reward processing; translational neuroscience; treatment effect; treatment response; virtual reality

DESCRIPTION (provided by applicant): Obsessive-Compulsive Disorder (OCD) is a disabling illness that typically begins in adolescence and persists into adulthood. We hypothesize that OCD is due to dysfunction in frontostriatal brain circuits that subserve self-regulatory control processes, and that these disturbances affect stimulus-response 'habit' learning systems within the dorsal striatum and declarative memory systems within medial temporal lobe regions that are components of a mesocorticolimbic reward processing system. In this R21, we will use fMRI to assess the functioning of these three neural systems in 30 unmedicated adults with OCD (ages 18-45) compared to 30 age-matched healthy controls (Primary Aim). The functioning of frontostriatal control systems will be assessed using the well-validated Simon task. The functioning of habit learning and reward processing systems will be assessed using a novel fMRI paradigm directly analogous to tasks used to define the neural bases of learning and memory systems in animal research, tailored to a virtual reality environment within the MRI scanner. This paradigm provides a translational neuroscience approach to the study of brain function in OCD. After scanning, OCD patients will be offered 12 weeks of open treatment with a serotonin reuptake inhibitor (SRI), and we will explore whether our baseline fMRI measures predict SRI response (Secondary Aim). Identification of functional abnormalities (a biosignature) in any of these neural systems in OCD will support future studies to investigate the onset and progression of these brain abnormalities and the effects of treatment. If these abnormalities are associated with treatment response, these fMRI paradigms could become valid biomarkers for OCD. Our long-term goal is to identify a distinct pattern of brain abnormalities that underlies OCD and/or predicts treatment response, and to develop novel treatments that target these abnormalities directly. By validating the use of specific fMRI paradigms to examine potential brain mechanisms underlying OCD, this R21 application is a first step in this direction and consistent with the NIMH strategic plan to promote brain discovery and to identify biomarkers of treatment response. PUBLIC HEALTH RELEVANCE: We propose to investigate functional abnormalities in three neural systems that we hypothesize underlie Obsessive-Compulsive Disorder (OCD) and to explore whether these abnormalities are associated with OCD severity and/or predict treatment response. Identification of abnormalities in these neural systems will not only foster a better understanding of what causes OCD, but also enable future studies to examine when and how people with OCD develop these brain abnormalities and to develop novel treatments that directly target them.

描述（由申请人提供）：强迫症（OCD）是一种致残性疾病，通常始于青春期并持续到成年。我们假设，强迫症是由于功能障碍的额纹状体的大脑回路，subserve自我调节控制过程，这些干扰影响刺激反应的“习惯”的学习系统在背侧纹状体和内侧颞叶区域内的陈述性记忆系统，是一个mesocorticolimbic奖励处理系统的组成部分。在这个R21中，我们将使用fMRI来评估这三个神经系统在30个未服药的成人强迫症（年龄18-45）与30个年龄匹配的健康对照（主要目的）的功能。将使用经过充分验证的Simon任务评估额纹状体控制系统的功能。习惯学习和奖励处理系统的功能将使用一种新的功能磁共振成像范式进行评估，该范式直接类似于用于定义动物研究中学习和记忆系统的神经基础的任务，适合于MRI扫描仪内的虚拟现实环境。这一范式为强迫症的脑功能研究提供了一种转化神经科学方法。扫描后，强迫症患者将接受12周的5-羟色胺再摄取抑制剂（SRI）开放治疗，我们将探讨我们的基线fMRI测量是否预测SRI反应（次要目标）。在强迫症的任何这些神经系统中识别功能异常（生物特征）将支持未来的研究，以调查这些大脑异常的发作和进展以及治疗效果。如果这些异常与治疗反应有关，这些功能磁共振成像范例可能成为有效的生物标志物强迫症。我们的长期目标是确定一个独特的模式，大脑异常的基础强迫症和/或预测治疗反应，并开发新的治疗方法，直接针对这些异常。通过验证使用特定的功能磁共振成像范例来检查强迫症潜在的大脑机制，R21的应用是朝着这个方向迈出的第一步，并且与NIMH促进大脑发现和识别治疗反应生物标志物的战略计划一致。 公共卫生关系：我们建议调查三个神经系统的功能异常，我们假设强迫症（OCD）的基础，并探讨这些异常是否与强迫症的严重程度和/或预测治疗反应。识别这些神经系统的异常不仅有助于更好地了解是什么导致了强迫症，而且还使未来的研究能够检查强迫症患者何时以及如何发展这些大脑异常，并开发直接针对它们的新治疗方法。