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脑振荡作为神经精神疾病的生物标志物:继一场互动小组讨论及概述之后

Brain oscillations as biomarkers in neuropsychiatric disorders: following an interactive panel discussion and synopsis.

作者信息

Yener Görsev G, Başar Erol

机构信息

Brain Dynamics Multidisciplinary Research Center, Dokuz Eylül University, Izmir 35340, Turkey.

出版信息

Suppl Clin Neurophysiol. 2013;62:343-63. doi: 10.1016/b978-0-7020-5307-8.00016-8.

Abstract

This survey covers the potential use of neurophysiological changes as a biomarker in four neuropsychiatric diseases (attention deficit hyperactivity disorder (ADHD), Alzheimer's disease (AD), bipolar disorder (BD), and schizophrenia (SZ)). Great developments have been made in the search of biomarkers in these disorders, especially in AD. Nevertheless, there is a tremendous need to develop an efficient, low-cost, potentially portable, non-invasive biomarker in the diagnosis, course, or treatment of the above-mentioned disorders. Electrophysiological methods would provide a tool that would reflect functional brain dynamic changes within milliseconds and also may be used as an ensemble of biomarkers that is greatly needed in the evaluation of cognitive changes seen in these disorders. The strategies for measuring cognitive changes include spontaneous electroencephalography (EEG), sensory evoked oscillation (SEO), and event-related oscillations (ERO). Further selective connectivity deficit in sensory or cognitive networks is reflected by coherence measurements. Possible candidate biomarkers discussed in an interactive panel can be summarized as follows: for ADHD: (a) elevation of delta and theta, (b) diminished alpha and beta responses in spontaneous EEG; for SZ: (a) decrease of ERO gamma responses, (b) decreased ERO in all other frequency ranges, (c) invariant ERO gamma response in relation to working memory demand; for euthymic BD: (a) decreased event-related gamma coherence, (b) decreased alpha in ERO and in spontaneous EEG; for manic BD: (a) lower alpha and higher beta in ERO, (b) decreased event-related gamma coherence, (c) lower alpha and beta in ERO after valproate; and for AD: (a) decreased alpha and beta, and increased theta and delta in spontaneous EEG, (b) hyperexcitability of motor cortices as shown by transcortical magnetic stimulation, (c) hyperexcitability of visual sensory cortex as indicated by increased SEO theta responses, (d) lower delta ERO, (e) lower delta, theta, and alpha event-related coherence, (f) higher theta synchrony and higher alpha event-related coherence in cholinergically treated AD subjects. In further research in the search for biomarkers, multimodal methods should be introduced to electrophysiology for validation purposes. Also, providing the protocols for standardization and harmonization of user-friendly acquisition or analysis methods that would be applied in larger cohort populations should be used to incorporate these electrophysiologic methods into the clinical criteria. In an extension to conventional anatomical, biochemical and brain imaging biomarkers, the use of neurophysiologic markers may lead to new applications for functional interpretrations and also the possibility to monitor treatments tailored for individuals.

摘要

本调查涵盖了神经生理变化作为生物标志物在四种神经精神疾病(注意力缺陷多动障碍(ADHD)、阿尔茨海默病(AD)、双相情感障碍(BD)和精神分裂症(SZ))中的潜在应用。在这些疾病的生物标志物研究方面已经取得了巨大进展,尤其是在AD方面。然而,在上述疾病的诊断、病程或治疗中,迫切需要开发一种高效、低成本、可能便于携带的非侵入性生物标志物。电生理方法将提供一种工具,能够在毫秒内反映大脑功能的动态变化,也可作为评估这些疾病中认知变化急需的一组生物标志物。测量认知变化的策略包括自发脑电图(EEG)、感觉诱发振荡(SEO)和事件相关振荡(ERO)。感觉或认知网络中进一步的选择性连接缺陷通过相干测量来反映。在一个互动小组中讨论的可能的候选生物标志物可总结如下:对于ADHD:(a)δ波和θ波升高,(b)自发EEG中α波和β波反应减弱;对于SZ:(a)EROγ反应降低,(b)所有其他频率范围内的ERO降低,(c)EROγ反应与工作记忆需求无关;对于心境正常的BD:(a)事件相关γ相干性降低,(b)ERO和自发EEG中的α波降低;对于躁狂BD:(a)ERO中的α波降低和β波升高,(b)事件相关γ相干性降低,(c)丙戊酸盐治疗后ERO中的α波和β波降低;对于AD:(a)自发EEG中α波和β波降低,θ波和δ波升高,(b)经颅磁刺激显示运动皮层兴奋性增高,(c)SEOθ反应增加表明视觉感觉皮层兴奋性增高,(d)δ波ERO降低,(e)δ波、θ波和α波事件相关相干性降低,(f)胆碱能治疗的AD患者中θ波同步性更高和α波事件相关相干性更高。在寻找生物标志物的进一步研究中,应将多模态方法引入电生理学以进行验证。此外,应提供用于标准化和统一用户友好的采集或分析方法的方案,这些方法将应用于更大的队列人群,以便将这些电生理方法纳入临床标准。在扩展传统的解剖、生化和脑成像生物标志物的基础上,使用神经生理标志物可能会带来功能解释的新应用,也有可能监测针对个体的治疗。

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