4.2 Article

Nonmotor Symptoms and Cognitive Decline in de novo Parkinson's Disease

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CANADIAN JOURNAL OF NEUROLOGICAL SCIENCES
卷 41, 期 5, 页码 597-602

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CANADIAN JOURNAL NEUROLOGICAL SCIENCES INC
DOI: 10.1017/cjn.2014.3

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Nonmotor symptoms; hyposmia; depression; stereopsis; dementia; Parkinson's disease

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Background: Cognitive impairments are common in Parkinson's disease (PD). Despite its clinical importance, the development of dementia is still difficult to predict. In this study, we investigated the possible associations between non-motor symptoms and the risk of developing dementia within a 2-year observation period in PD. Methods: A total of 80 patients with PD participated in this study. Nonmotor symptoms (the Nonmotor Symptoms Questionnaire), PD status (Unified Parkinson's Disease Rating Scale), depression (Geriatric d Depression Scale or Montgomery-Asberg Depression Scale), stereopsis and severity of nonmotor symptoms (Non-motor symptoms scale) were assessed. Global cognitive function (Mini-Mental State Examination) were evaluated at baseline and 2 years later. Results: Presence of depression, vivid dreaming, REM sleep behavior disorders, hyposmia, abnormal stereopsis, non-smoking and postural instability/gait disturbance phenotype were associated with a significantly more rapid decline of Mini-Mental State Examination. Logistic regression analyses demonstrated that depression (odds ratio = 13.895), abnormal stereopsis (odds ratio = 10.729), vivid dreaming (odds ratio = 4.16), REM sleep behavior disorders (odds ratio = 5.353) and hyposmia (odds ratio = 4.911) were significant independent predictors of dementia risk within 2 years. Postural instability/gait disturbance phenotype and age >62 years were also independent predictors of dementia risk (odd ratio = 38.333, odds ratio = 10.625). Conclusions: We suggest that depression, vivid dreaming, REM sleep behavior disorders, hyposmia and abnormal stereopsis are closely associated with cognitive decline, and that presence of these nonmotor symptoms predict the subsequent development of Parkinson's disease dementia.

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