Two-year clinical progression in focal and diffuse subtypes of Parkinson’s disease

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作者
Martin E. Johansson
Nina M. van Lier
Roy P. C. Kessels
Bastiaan R. Bloem
Rick C. Helmich
机构
[1] Radboud University,Centre for Cognitive Neuroimaging, Donders Institute for Brain, Cognition and Behaviour
[2] Radboud University,Centre for Medical Neuroscience, Donders Institute for Brain, Cognition and Behaviour
[3] Radboud University Medical Center,Center of Expertise for Parkinson & Movement Disorders, Department of Neurology
[4] Radboud University,Donders Institute for Brain, Cognition and Behaviour
[5] Radboud University Medical Center,Department of Medical Psychology
[6] ,Radboudumc Alzheimer Center
[7] Radboud University Medical Center,undefined
[8] Vincent van Gogh Institute for Psychiatry,undefined
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摘要
Heterogeneity in Parkinson’s disease (PD) presents a barrier to understanding disease mechanisms and developing new treatments. This challenge may be partially overcome by stratifying patients into clinically meaningful subtypes. A recent subtyping scheme classifies de novo PD patients into three subtypes: mild-motor predominant, intermediate, or diffuse-malignant, based on motor impairment, cognitive function, rapid eye movement sleep behavior disorder (RBD) symptoms, and autonomic symptoms. We aimed to validate this approach in a large longitudinal cohort of early-to-moderate PD (n = 499) by assessing the influence of subtyping on clinical characteristics at baseline and on two-year progression. Compared to mild-motor predominant patients (42%), diffuse-malignant patients (12%) showed involvement of more clinical domains, more diffuse hypokinetic-rigid motor symptoms (decreased lateralization and hand/foot focality), and faster two-year progression. These findings extend the classification of diffuse-malignant and mild-motor predominant subtypes to early-to-moderate PD and suggest that different pathophysiological mechanisms (focal versus diffuse cerebral propagation) may underlie distinct subtype classifications.
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