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Advances in markers of prodromal Parkinson disease

机译:前驱性帕金森病标志物的研究进展

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摘要

Efforts to develop neuroprotective therapy for Parkinson disease (PD) are focusing on the early stages of disease, which offer the best opportunity to intervene. Early PD can be divided into preclinical, prodromal and clinical stages; in this Review, we focus on the prodromal stage and markers that can be used to identify prodromal PD. We consider the necessary properties of a marker, before providing an overview of the proven and potential markers of prodromal PD, including clinical nonmotor markers, clinical motor markers, neuroimaging markers and tissue biomarkers. Markers for which the ability to predict conversion to PD is supported by the strongest evidence include olfactory loss, REM sleep behaviour disorder and constipation. Markers with the highest diagnostic strength include REM sleep behaviour disorder, dopaminergic imaging and subtle motor parkinsonism. The lead time-the period between the appearance of a marker and conversion to PD-is highly variable between markers, ranging from 5 years for impaired motor performance to > 20 years for autonomic symptoms. The cost of screening for these markers also varies dramatically: some require just questionnaires, whereas others require sophisticated scanning techniques. Finally, we summarize how prodromal and risk markers can be combined to estimate the probability that an individual has prodromal PD, with a focus on the International Parkinson Disease and Movement Disorders Society (MDS) Prodromal Parkinson Criteria.
机译:开发针对帕金森氏病(PD)的神经保护疗法的工作集中在疾病的早期阶段,这为干预提供了最佳机会。早期PD可分为临床前,驱原和临床阶段。在本综述中,我们集中于前驱阶段和可用于识别前驱PD的标记物。在概述前驱性PD的可靠和潜在标记之前,我们考虑标记的必要属性,包括临床非运动标记,临床运动标记,神经影像标记和组织生物标记。最有力的证据支持其预测转化为PD的能力的标记包括嗅觉丧失,REM睡眠行为障碍和便秘。诊断强度最高的标志物包括REM睡眠行为障碍,多巴胺能显像和微妙的运动帕金森综合症。前置时间(标志物出现与转化为PD之间的时间)在标志物之间变化很大,范围从运动能力受损的5年到自主神经症状的> 20年。筛选这些标记物的成本也相差很大:有些仅需要问卷,而另一些则需要复杂的扫描技术。最后,我们总结了如何结合前驱和危险标记物来估计个人患有前驱PD的可能性,重点是国际帕金森疾病和运动障碍协会(MDS)前驱帕金森标准。

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