Anatomical abnormalities suggest a compensatory role of the cerebellum in early Parkinson's disease

IF 4.5 2区 医学 Q1 NEUROIMAGING NeuroImage Pub Date : 2025-03-05 DOI:10.1016/j.neuroimage.2025.121121
Juyoung Jenna Yun , Anastasia Gailly de Taurines , Yen F Tai , Shlomi Haar
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Abstract

Brain atrophy is detected in early Parkinson's disease (PD) and accelerates over the first few years post-diagnosis. This was captured by multiple cross-sectional studies and a few longitudinal studies in early PD. Yet only a longitudinal study with a control group can capture accelerated atrophy in early PD and differentiate it from healthy ageing. Accordingly, we performed a multicohort longitudinal analysis between PD and healthy ageing, examining subcortical regions implicated in PD pathology, including the basal ganglia, thalamus, corpus callosum (CC), and cerebellum. Longitudinal volumetric analysis was performed on 56 early PD patients and 53 matched controls, with scans collected 2–3 years apart. At baseline, the PD group showed a greater volume in the pallidum, thalamus, and cerebellar white matter (WM), suggesting potential compensatory mechanisms in prodromal and early PD. After 2–3 years, accelerated atrophy in PD was observed in the putamen and cerebellar WM. Interestingly, healthy controls – but not PD patients – demonstrated a significant decline in Total Intracranial Volume (TIV), and atrophy in the thalamus and mid-CC. Between-group analysis revealed more severe atrophy in the right striatum and cerebellar WM in PD, and in the mid-posterior CC in controls. Using CEREbellum Segmentation (CERES) for lobule segmentation on the longitudinal PD cohort, we found a significant decline in the WM of non-motor regions in the cerebellum, specifically Crus I and lobule IX. Our results highlight an initial increase in cerebellar WM volume during prodromal PD, followed by significant degeneration over the first few years post-diagnosis.
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解剖异常表明小脑在早期帕金森病中起着代偿作用
脑萎缩在早期帕金森病(PD)中被检测到,并在诊断后的头几年加速。这在早期PD的多个横断面研究和一些纵向研究中得到了证实。然而,只有一项与对照组的纵向研究才能捕捉到早期帕金森病的加速萎缩,并将其与健康衰老区分开来。因此,我们进行了PD与健康老龄化之间的多队列纵向分析,检查了与PD病理相关的皮质下区域,包括基底神经节、丘脑、胼胝体(CC)和小脑。对56名早期PD患者和53名匹配对照进行纵向体积分析,扫描间隔2-3年。在基线时,PD组在苍白球、丘脑和小脑白质(WM)中显示出更大的体积,这表明在前驱期和早期PD中可能存在代偿机制。2-3年后,PD患者的壳核和小脑WM加速萎缩。有趣的是,健康对照组——而不是PD患者——表现出总颅内容积(TIV)的显著下降,以及丘脑和中cc的萎缩。组间分析显示,PD患者右侧纹状体和小脑WM萎缩更为严重,对照组中后侧CC萎缩更为严重。在纵向PD队列中使用小脑分割(CERES)进行小叶分割,我们发现小脑非运动区域的WM显著下降,特别是小腿I和小叶IX。我们的研究结果强调了PD前驱期小脑WM体积的初始增加,随后在诊断后的最初几年出现了明显的变性。
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来源期刊
NeuroImage
NeuroImage 医学-核医学
CiteScore
11.30
自引率
10.50%
发文量
809
审稿时长
63 days
期刊介绍: NeuroImage, a Journal of Brain Function provides a vehicle for communicating important advances in acquiring, analyzing, and modelling neuroimaging data and in applying these techniques to the study of structure-function and brain-behavior relationships. Though the emphasis is on the macroscopic level of human brain organization, meso-and microscopic neuroimaging across all species will be considered if informative for understanding the aforementioned relationships.
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