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神经生理学生物标志物在精神分裂症治疗反应预测和监测中的未来临床应用。

Future clinical uses of neurophysiological biomarkers to predict and monitor treatment response for schizophrenia.

作者信息

Light Gregory A, Swerdlow Neal R

机构信息

VISN 22 Mental Illness, Research, Education, and Clinical Center (MIRECC), VA San Diego Healthcare System, San Diego, California; Department of Psychiatry, University of California San Diego, La Jolla, California.

出版信息

Ann N Y Acad Sci. 2015 May;1344(1):105-19. doi: 10.1111/nyas.12730. Epub 2015 Mar 9.

Abstract

Advances in psychiatric neuroscience have transformed our understanding of impaired and spared brain functions in psychotic illnesses. Despite substantial progress, few (if any) laboratory tests have graduated to clinics to inform diagnoses, guide treatments, and monitor treatment response. Providers must rely on careful behavioral observation and interview techniques to make inferences about patients' inner experiences and then secondary deductions about impacted neural systems. Development of more effective treatments has also been hindered by a lack of translational quantitative biomarkers that can span the brain-behavior treatment knowledge gap. Here, we describe an example of a simple, low-cost, and translatable electroencephalography (EEG) measure that offers promise for improving our understanding and treatment of psychotic illnesses: mismatch negativity (MMN). MMN is sensitive to and/or predicts response to some pharmacologic and nonpharmacologic interventions and accounts for substantial portions of variance in clinical, cognitive, and psychosocial functioning in schizophrenia (SZ). This measure has recently been validated for use in large-scale multisite clinical studies of SZ. Finally, MMN greatly improves our ability to forecast which individuals at high clinical risk actually develop a psychotic illness. These attributes suggest that MMN can contribute to personalized biomarker-guided treatment strategies aimed at ameliorating or even preventing the onset of psychosis.

摘要

精神神经科学的进展改变了我们对精神病性疾病中受损和未受损脑功能的理解。尽管取得了重大进展,但很少有(如果有的话)实验室检测能够进入临床,为诊断提供依据、指导治疗并监测治疗反应。医疗服务提供者必须依靠仔细的行为观察和访谈技巧来推断患者的内心体验,进而对受影响的神经系统进行二次推断。由于缺乏能够跨越脑 - 行为治疗知识鸿沟的可转化定量生物标志物,更有效治疗方法的开发也受到了阻碍。在此,我们描述了一种简单、低成本且可转化的脑电图(EEG)测量方法的示例,它有望改善我们对精神病性疾病的理解和治疗:失配负波(MMN)。MMN 对某些药物和非药物干预敏感并 / 或能预测其反应,且在精神分裂症(SZ)的临床、认知和社会心理功能变异中占很大比例。该测量方法最近已在 SZ 的大规模多中心临床研究中得到验证。最后,MMN 极大地提高了我们预测哪些处于高临床风险的个体实际上会发展为精神病性疾病的能力。这些特性表明,MMN 有助于制定个性化的生物标志物指导治疗策略,旨在改善甚至预防精神病的发作。

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