阿尔茨海默病病理生理过程的追踪:动态生物标志物的更新假设模型。
Tracking pathophysiological processes in Alzheimer's disease: an updated hypothetical model of dynamic biomarkers.
机构信息
Department of Radiology, Mayo Clinic, Rochester, MN 55905, USA.
出版信息
Lancet Neurol. 2013 Feb;12(2):207-16. doi: 10.1016/S1474-4422(12)70291-0.
Abstract
In 2010, we put forward a hypothetical model of the major biomarkers of Alzheimer's disease (AD). The model was received with interest because we described the temporal evolution of AD biomarkers in relation to each other and to the onset and progression of clinical symptoms. Since then, evidence has accumulated that supports the major assumptions of this model. Evidence has also appeared that challenges some of our assumptions, which has allowed us to modify our original model. Refinements to our model include indexing of individuals by time rather than clinical symptom severity; incorporation of interindividual variability in cognitive impairment associated with progression of AD pathophysiology; modifications of the specific temporal ordering of some biomarkers; and recognition that the two major proteinopathies underlying AD biomarker changes, amyloid β (Aβ) and tau, might be initiated independently in sporadic AD, in which we hypothesise that an incident Aβ pathophysiology can accelerate antecedent limbic and brainstem tauopathy.
摘要
2010 年,我们提出了阿尔茨海默病(AD)主要生物标志物的假设模型。该模型受到了关注,因为我们描述了 AD 生物标志物彼此之间以及与临床症状的发生和进展之间的时间演变。从那时起,越来越多的证据支持该模型的主要假设。也出现了一些挑战我们某些假设的证据,这使我们能够修改我们的原始模型。对我们模型的改进包括根据时间而不是临床症状严重程度对个体进行索引;将与 AD 病理生理学进展相关的认知障碍的个体间变异性纳入其中;修改一些生物标志物的特定时间顺序;并认识到导致 AD 生物标志物变化的两种主要蛋白病,β淀粉样蛋白(Aβ)和 tau,可能在散发性 AD 中独立发生,我们假设,Aβ 病理生理学的偶发事件可以加速先前的边缘和脑干 tau 病。
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