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精神分裂症的神经生理内表型:所选候选测量方法的可行性

Neurophysiological endophenotypes of schizophrenia: the viability of selected candidate measures.

作者信息

Turetsky Bruce I, Calkins Monica E, Light Gregory A, Olincy Ann, Radant Allen D, Swerdlow Neal R

机构信息

Department of Psychiatry, 10th floor, Gates Building, University of Pennsylvania, 3400 Spruce Street, Philadelphia, PA 19104, USA.

出版信息

Schizophr Bull. 2007 Jan;33(1):69-94. doi: 10.1093/schbul/sbl060. Epub 2006 Nov 29.

Abstract

In an effort to reveal susceptibility genes, schizophrenia research has turned to the endophenotype strategy. Endophenotypes are characteristics that reflect the actions of genes predisposing an individual to a disorder, even in the absence of diagnosable pathology. Individual endophenotypes are presumably determined by fewer genes than the more complex phenotype of schizophrenia and would, therefore, reduce the complexity of genetic analyses. Unfortunately, despite there being rational criteria to define a viable endophenotype, the term is sometimes applied indiscriminately to characteristics that are deviant in affected individuals. Schizophrenia patients exhibit deficits in several neurophysiological measures of information processing that have been proposed as candidate endophenotypes. Successful processing of sensory inputs requires the ability to inhibit intrinsic responses to redundant stimuli and, reciprocally, to facilitate responses to less frequent salient stimuli. There is evidence to suggest that both these processes are "impaired" in schizophrenia. Measures of inhibitory failure include prepulse inhibition of the startle reflex, P50 auditory evoked potential suppression, and antisaccade eye movements. Measures of impaired deviance detection include mismatch negativity and the P300 event-related potential. The purpose of this review is to systematically evaluate the endophenotype candidacy of these key neurophysiological abilities. For each candidate, we describe typical experimental procedures, the current understanding of the underlying neurobiology, the nature of the abnormality in schizophrenia, the reliability, stability and heritability of the measure, and any reported gene associations. We conclude with a discussion of the few studies thus far that have employed a multivariate approach with these candidates.

摘要

为了揭示易感基因,精神分裂症研究已转向内表型策略。内表型是指即使在没有可诊断病理的情况下,也能反映使个体易患某种疾病的基因作用的特征。与精神分裂症这种更复杂的表型相比,单个内表型可能由较少的基因决定,因此可以降低遗传分析的复杂性。不幸的是,尽管有合理的标准来定义可行的内表型,但这个术语有时会被不加区分地应用于受影响个体中出现异常的特征。精神分裂症患者在几种信息处理的神经生理学测量中表现出缺陷,这些测量已被提议作为候选内表型。成功处理感觉输入需要能够抑制对冗余刺激的内在反应,反之,促进对较少出现的显著刺激的反应。有证据表明,在精神分裂症中这两个过程都“受损”。抑制失败的测量包括惊吓反射的前脉冲抑制、P50听觉诱发电位抑制和反扫视眼动。异常检测受损的测量包括失配负波和P300事件相关电位。本综述的目的是系统评估这些关键神经生理能力作为内表型的可能性。对于每个候选指标,我们描述了典型的实验程序、对潜在神经生物学的当前理解、精神分裂症中异常的性质、测量的可靠性、稳定性和遗传性,以及任何已报道的基因关联。我们最后讨论了迄今为止少数几项对这些候选指标采用多变量方法的研究。

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