Jellinger Kurt A, Attems Johannes
Institute of Clinical Neurobiology, Vienna, Austria.
Acta Neuropathol. 2008 Apr;115(4):427-36. doi: 10.1007/s00401-008-0347-5. Epub 2008 Feb 14.
Whereas the prevalence and impact of vascular pathology in Alzheimer diease (AD) are well established, the role of vascular and Alzheimer pathologies in the progression of neurodegeneration and cognitive impairment in Parkinson disease (PD) is under discussion. A retrospective clinico-pathologic study of 100 patients with autopsy proven PD (including 44 cases with dementia/PDD) and 20 cases of dementia with Lewy bodies (DLB) confirmed essential clinical (duration of illness, Mini-Mental State Examination/MMSE, age at death) and morphologic differences between these groups; Lewy body Braak scores and Alzheimer pathologies (neuritic Braak stage, cortical Abeta plaque load, and generalized cerebral amyloid angiopathy or CAA) were significantly higher/more severe in DLB and PDD than in PD without dementia. Duration of illness showed no association to any of the examined pathologic parameters, while there was a moderate association between LB scores and neuritic Braak stages, the latter significantly increasing with age. Significant association between cerebrovascular lesions and neuritic Braak stage was seen in PDD but not in PD subjects without dementia. These data suggest an influence of Alzheimer-related lesions on the progression of the neurodegenerative process and, in particular, on cognitive decline in both PDD and DLB. On the other hand, both these factors in PD and DLB appear to be largely independent from coexistent vascular pathology, except in cases with severe cerebrovascular lesions or those related to neuritic AD pathology. Assessment of ApoE genotype in a small number of cases showed no significant differences in the severity of Abeta plaque load and CAA except for much lower intensities in non-demented epsilon3/3 patients. Despite increasing evidence suggesting synergistic reactions between alpha-synuclein (alphaSyn), tau and Abeta-peptides, the major protein markers of both AD and Lewy body diseases, and of both vascular pathology and AD, the molecular background and pathophysiological impact of these pathologies on the progression of neurodegeneration and development of cognitive decline in PD await further elucidation.
虽然血管病变在阿尔茨海默病(AD)中的患病率和影响已得到充分证实,但血管病变和阿尔茨海默病病理在帕金森病(PD)神经退行性变和认知障碍进展中的作用仍在讨论中。一项对100例经尸检证实为PD的患者(包括44例痴呆/帕金森病痴呆症患者)和20例路易体痴呆(DLB)患者的回顾性临床病理研究证实了这些组之间在基本临床特征(病程、简易精神状态检查表/MMSE、死亡年龄)和形态学上的差异;DLB和帕金森病痴呆症患者的路易体Braak评分和阿尔茨海默病病理(神经炎性Braak分期、皮质β淀粉样蛋白斑块负荷和全身性脑淀粉样血管病或CAA)明显高于/重于无痴呆的PD患者。病程与任何检查的病理参数均无关联,而路易体评分与神经炎性Braak分期之间存在中度关联,后者随年龄显著增加。在帕金森病痴呆症患者中观察到脑血管病变与神经炎性Braak分期之间存在显著关联,但在无痴呆的PD患者中未观察到。这些数据表明,阿尔茨海默病相关病变对神经退行性变过程的进展有影响,特别是对帕金森病痴呆症和DLB患者的认知衰退有影响。另一方面,PD和DLB中的这两个因素似乎在很大程度上独立于共存的血管病变,除非是严重脑血管病变或与神经炎性AD病理相关的病例。对少数病例的载脂蛋白E基因型评估显示,除了非痴呆的ε3/3患者强度低得多外,β淀粉样蛋白斑块负荷和CAA的严重程度没有显著差异。尽管越来越多的证据表明α-突触核蛋白(αSyn)、tau和β淀粉样肽之间存在协同反应,这些肽是AD和路易体病以及血管病变和AD的主要蛋白质标志物,但这些病变对PD神经退行性变进展和认知衰退发展的分子背景和病理生理影响仍有待进一步阐明。
