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首页> 外文期刊>NeuroImage >A novel method for noninvasive detection of neuromodulatory changes in specific neurotransmitter systems.
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A novel method for noninvasive detection of neuromodulatory changes in specific neurotransmitter systems.

机译:一种用于非侵入性检测特定神经递质系统中神经调节变化的新方法。

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摘要

Over the last decade, it has become possible to study theories of cognition using positron emission tomography (PET) and functional magnetic resonance imaging (fMRI). These methods yield statistical parametric maps of changes in cerebral blood flow (CBF) elicited by cognitive tasks. A limitation of these studies is that they provide no information about the underlying neurochemistry. However, it is possible to extend the concept of activation studies to include measurements targeting neurotransmitters and specific receptor populations. Cognitive activation increases neuronal firing rate, increasing the endogenous neurotransmitter level. The increased neurotransmitter level can be used to alter the kinetics of specifically bound radioligands. We describe a new approach to the design and analysis of neuromodulation experiments. This approach uses PET, a single-scan session design, and a linear extension of the simplified reference region model (LSSRM) that accounts for changes in ligand binding induced by cognitive tasks or drug challenge. In the LSSRM, an activation of change in apparent dissociation rate. Activation of the neurotransmitter is detected statistically when the activation parameter is shown to violate the null hypothesis. Simulation was used to explore the properties of the LSSRM with regard to model identifiability, effect of statistical noise, and confounding effects of CBF-related changes. Simulation predicted that it is possible to detect and map neuromodulatory changes in single-subject designs. A human study was conducted to confirm the predictions of simulation using (11)C-raclopride and a motor planning task. Parametric images of transport, binding potential, areas of significant dopamine release, and statistical parameters were computed. Examination of the kinetics of activation demonstrated that maximum dopamine release occurred immediately following task initiation and then decreased with a half-time of about 3 min. This method can be extended to explore neurotransmitter involvement in other behavioral and cognitive domains.
机译:在过去的十年中,使用正电子发射断层扫描(PET)和功能磁共振成像(fMRI)研究认知理论成为可能。这些方法产生认知任务引起的脑血流量(CBF)变化的统计参数图。这些研究的局限性在于它们不提供有关潜在神经化学的信息。但是,可以将激活研究的概念扩展到包括针对神经递质和特定受体群体的测量。认知激活会增加神经元放电速度,从而增加内源性神经递质水平。增加的神经递质水平可用于改变特异性结合的放射性配体的动力学。我们描述了一种新的方法来设计和分析神经调节实验。该方法使用PET,单次扫描会话设计和简化的参考区域模型(LSSRM)的线性扩展,该模型可解释由于认知任务或药物挑战引起的配体结合变化。在LSSRM中,表观解离速率变化的激活。当显示激活参数违反原假设时,可以统计地检测到神经递质的激活。仿真用于探讨LSSRM在模型可识别性,统计噪声的影响以及CBF相关变化的混杂影响方面的属性。仿真预测,可以检测和映射单受试者设计中的神经调节变化。进行了一项人为研究,以确认使用(11)C-雷氯必利和一项运动计划任务进行模拟的预测。计算运输,结合潜力,多巴胺释放的面积和统计参数的参数图像。激活动力学的研究表明,最大的多巴胺释放在任务开始后立即发生,然后以约3分钟的半衰期降低。该方法可以扩展为探索其他行为和认知领域中神经递质的参与。

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