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将 EEG 用作替代生物标志物的策略:临床前和临床研究综述。

Aligning strategies for using EEG as a surrogate biomarker: a review of preclinical and clinical research.

机构信息

Synaptic Transmission, Lundbeck Research USA, Inc., 215 College Road, Paramus, NJ 07652, United States.

出版信息

Biochem Pharmacol. 2011 Jun 15;81(12):1408-21. doi: 10.1016/j.bcp.2010.10.002. Epub 2010 Oct 19.

DOI:10.1016/j.bcp.2010.10.002
PMID:20937262
Abstract

Electroencephalography (EEG) and related methodologies offer the promise of predicting the likelihood that novel therapies and compounds will exhibit clinical efficacy early in preclinical development. These analyses, including quantitative EEG (e.g. brain mapping) and evoked/event-related potentials (EP/ERP), can provide a physiological endpoint that may be used to facilitate drug discovery, optimize lead or candidate compound selection, as well as afford patient stratification and Go/No-Go decisions in clinical trials. Currently, the degree to which these different methodologies hold promise for translatability between preclinical models and the clinic have not been well summarized. To address this need, we review well-established and emerging EEG analytic approaches that are currently being integrated into drug discovery programs throughout preclinical development and clinical research. Furthermore, we present the use of EEG in the drug development process in the context of a number of major central nervous system disorders including Alzheimer's disease, schizophrenia, depression, attention deficit hyperactivity disorder, and pain. Lastly, we discuss the requirements necessary to consider EEG technologies as a biomarker. Many of these analyses show considerable translatability between species and are used to predict clinical efficacy from preclinical data. Nonetheless, the next challenge faced is the selection and validation of EEG endpoints that provide a set of robust and translatable biomarkers bridging preclinical and clinical programs.

摘要

脑电图(EEG)和相关方法有望预测新疗法和化合物在临床前开发早期是否具有临床疗效。这些分析,包括定量脑电图(如脑映射)和诱发/事件相关电位(EP/ERP),可以提供一个生理终点,可用于促进药物发现、优化先导化合物或候选化合物的选择,并在临床试验中进行患者分层和是否继续的决策。目前,这些不同方法在临床前模型和临床之间的转化潜力程度尚未得到很好的总结。为了解决这一需求,我们回顾了目前正在整个临床前开发和临床研究中纳入药物发现计划的成熟和新兴的 EEG 分析方法。此外,我们还介绍了 EEG 在包括阿尔茨海默病、精神分裂症、抑郁症、注意缺陷多动障碍和疼痛在内的一些主要中枢神经系统疾病的药物开发过程中的应用。最后,我们讨论了将 EEG 技术作为生物标志物考虑的必要条件。这些分析中有许多在物种间具有相当的可转移性,并用于从临床前数据预测临床疗效。然而,下一个面临的挑战是选择和验证 EEG 终点,这些终点提供了一组稳健且可转化的生物标志物,将临床前和临床计划联系起来。

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