路易体病的皮质变薄的地形学。
Topography of cortical thinning in the Lewy body diseases.
机构信息
Department of Neurology, Massachusetts General Hospital, Charlestown, MA, USA.
Department of Neurology, Massachusetts General Hospital, Charlestown, MA, USA; Athinoula A. Martinos Center for Biomedical Imaging, Massachusetts General Hospital, Charlestown, MA, USA.
出版信息
Neuroimage Clin. 2020;26:102196. doi: 10.1016/j.nicl.2020.102196. Epub 2020 Jan 31.
OBJECTIVE
Regional cortical thinning in dementia with Lewy bodies (DLB) and Parkinson disease dementia (PDD) may underlie some aspect of their clinical impairments; cortical atrophy likely reflects extensive Lewy body pathology with alpha-synuclein deposits, as well as associated Alzheimer's disease co-pathologies, when present. Here we investigated the topographic distribution of cortical thinning in these Lewy body diseases compared to cognitively normal PD and healthy non-PD control subjects, explored the association of regional thinning with clinical features and evaluated the impact of amyloid deposition.
METHODS
Twenty-one participants with dementia with Lewy bodies (DLB), 16 with Parkinson disease (PD) - associated cognitive impairment (PD-MCI and PDD), and 24 cognitively normal participants with PD underwent MRI, PiB PET, and clinical evaluation. Cortical thickness across the brain and in regions of interest (ROIs) was compared across diagnostic groups and across subgroups stratified by amyloid status, and was related to clinical and cognitive measures.
RESULTS
DLB and PD-impaired groups shared a similar distribution of cortical thinning that included regions characteristic of AD, as well as the fusiform, precentral, and paracentral gyri. Elevated PiB retention in DLB and PD-impaired but not in PD-normal participants was associated with more extensive and severe cortical thinning, in an overlapping topography that selectively affected the medial temporal lobe in DLB participants. In DLB, greater thinning in AD signature and fusiform regions was associated with greater cognitive impairment.
CONCLUSIONS
The pattern of cortical thinning is similar in DLB and PD-associated cognitive impairment, overlapping with and extending beyond AD signature regions to involve fusiform, precentral, and paracentral regions. Cortical thinning in AD signature and fusiform regions in these diseases reflects cognitive impairment and is markedly accentuated by amyloid co-pathology. Further work will be required to determine whether the distinct topography of cortical thinning in DLB and PD-associated cognitive impairment might have value as a diagnostic and/ or outcome biomarker in clinical trials.
目的
路易体痴呆(DLB)和帕金森病痴呆(PDD)患者的区域性皮质变薄可能是其临床障碍的某些方面的基础;当存在时,皮质萎缩可能反映了广泛的路易体病理学,包括α-突触核蛋白沉积,以及相关的阿尔茨海默病共病。在这里,我们研究了这些路易体疾病与认知正常的 PD 和健康非 PD 对照组相比,皮质变薄的拓扑分布,探讨了区域变薄与临床特征的相关性,并评估了淀粉样蛋白沉积的影响。
方法
21 名痴呆性路易体病(DLB)患者、16 名帕金森病(PD)相关认知障碍(PD-MCI 和 PDD)患者和 24 名认知正常的 PD 患者接受了 MRI、PiB PET 和临床评估。比较了诊断组之间以及根据淀粉样蛋白状态分层的亚组之间的大脑和感兴趣区域(ROI)的皮质厚度,并与临床和认知测量相关。
结果
DLB 和 PD 受损组共享相似的皮质变薄分布,包括 AD 特征区域,以及梭状回、中央前回和中央旁回。DLB 和 PD 受损但 PD 正常参与者的 PiB 保留增加与更广泛和更严重的皮质变薄相关,重叠的拓扑选择性地影响了 DLB 参与者的内侧颞叶。在 DLB 中,AD 特征和梭状回区域的更大变薄与更大的认知障碍相关。
结论
DLB 和 PD 相关认知障碍的皮质变薄模式相似,重叠并扩展到 AD 特征区域以外,涉及梭状回、中央前回和中央旁回。这些疾病中 AD 特征和梭状回区域的皮质变薄反映了认知障碍,并因淀粉样蛋白共病而明显加重。需要进一步的工作来确定 DLB 和 PD 相关认知障碍的皮质变薄的独特拓扑是否可能作为临床试验中的诊断和/或预后生物标志物具有价值。
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