图雷特综合征相关的临床前模型。

Advances in neurology Pub Date : 2006-01-01
Neal R Swerdlow, Ashley N Sutherland
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引用次数: 0

摘要

如果使用得当,临床前模型可以大大加快对神经精神疾病的理解。许多动物模型对抗多巴胺能化合物具有预测有效性,这些抗多巴胺能化合物传统上用于抑制TS中的运动和声音抽搐。其他模型已被提出,可能对TS的感染/免疫和神经回路病因的特定假设具有构建有效性。基于TS的主要症状,包括感觉抽搐和先兆冲动,描述了一套更全面的模型。由调节感觉运动门控的脑机制功能障碍引起。这些模型利用中枢门控机制的操作措施,包括惊吓反射的PPI,来实现对许多不同化学类药物的预测效度,并在TS的神经发育、免疫和遗传病因的广泛领域实现构建效度。基于PPI的动物模型为TS的预测和机制研究提供了许多强大的优势。这些“缺陷门控”模型的效用将通过它们使我们更接近于确定这种疾病的原因和有效治疗的能力来判断。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Preclinical models relevant to Tourette syndrome.

Preclinical models, if used appropriately, can greatly accelerate the understanding of neuropsychiatric disorders. A number of animal models have predictive validity for antidopaminergic compounds that have traditionally been used to suppress motor and vocal tics in TS. Other models have been proposed that may have construct validity for specific hypotheses of infectious/immune and neural circuit etiologies of TS. A more comprehensive set of models is described, based on the hypothesis that primary symptoms of TS, including sensory tics and premonitory urges, result from dysfunction in brain mechanisms that regulate sensorimotor gating. These models utilize operational measures of central gating mechanisms, including PPI of the startle reflex, to achieve predictive validity across a number of different chemical classes of drugs, and to achieve construct validity across broad domains of neurodevelopmental, immune and genetic etiologies of TS. PPI-based animal models offer a number of strong advantages for predictive and mechanistic studies of TS. Ultimately, the utility of these "deficient gating" models will be judged by their ability to bring us closer to identifying the causes and effective treatments of this disorder.

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