Maruyama Masahiro, Matsui Toshifumi, Tanji Haruko, Nemoto Miyako, Tomita Naoki, Ootsuki Mari, Arai Hiroyuki, Sasaki Hidetada
Department of Geriatric Medicine, Tohoku University School of Medicine, Sendai, Miyagi, Japan.
Arch Neurol. 2004 May;61(5):716-20. doi: 10.1001/archneur.61.5.716.
Mild cognitive impairment (MCI) may be a heterogeneous condition rather than a uniform disease entity.
To develop reliable tools that aid in identifying patients at risk of developing Alzheimer disease (AD) among heterogeneous populations with MCI to maximize the benefits of emerging therapies for AD.
A 2-year prospective study.
Clinical follow-up in an outpatient memory clinic.
Seventy-two consecutive older patients with memory complaints.
Cerebrospinal fluid tau levels, severity of periventricular and deep white matter lesions, silent brain infarction on magnetic resonance imaging, plasma homocysteine levels, apolipoprotein E genotype, and other vascular risk factors were assessed at baseline.
Fifty-seven patients were diagnosed as having amnestic MCI. Forty-one patients with (AD-converted MCI group) or without (progressive MCI group) conversion to dementia and AD progressed over time, whereas the other 16 patients remained cognitively stable (stable MCI group). The stable MCI group was characterized by normal cerebrospinal fluid tau levels and a high grade of periventricular white matter lesions (PWMLs). The progressive MCI and AD-converted MCI groups had increased cerebrospinal fluid tau levels and low grades of PWMLs. A logistic regression model showed that age was significantly associated with developing PWMLs (P =.03; odds ratio, 1.15; 95% confidence interval, 1.0-1.3).
Tau-related AD pathologic conditions and possibly ischemic PWMLs represent 2 major etiologies in the development of MCI, reflecting heterogeneity in the clinical progression. Because the progressive type of MCI may be a primary target of clinical trials that aim at secondary prevention of dementia, these patients should be identified by appropriate biomarkers and neuroimaging techniques.
轻度认知障碍(MCI)可能是一种异质性疾病,而非单一的疾病实体。
开发可靠的工具,以帮助在患有MCI的异质性人群中识别有患阿尔茨海默病(AD)风险的患者,从而最大限度地提高AD新兴疗法的益处。
一项为期2年的前瞻性研究。
门诊记忆诊所的临床随访。
72例连续的有记忆障碍主诉的老年患者。
在基线时评估脑脊液tau水平、脑室周围和深部白质病变的严重程度、磁共振成像上的无症状脑梗死、血浆同型半胱氨酸水平、载脂蛋白E基因型及其他血管危险因素。
57例患者被诊断为遗忘型MCI。41例发生(AD转化型MCI组)或未发生(进行性MCI组)痴呆转化且AD随时间进展,而其他16例患者认知保持稳定(稳定MCI组)。稳定MCI组的特征是脑脊液tau水平正常且脑室周围白质病变(PWMLs)程度较高。进行性MCI组和AD转化型MCI组脑脊液tau水平升高且PWMLs程度较低。逻辑回归模型显示,年龄与PWMLs的发生显著相关(P = 0.03;比值比,1.15;95%置信区间,1.0 - 1.3)。
与tau相关的AD病理状况以及可能的缺血性PWMLs是MCI发生发展的2个主要病因,反映了临床进展的异质性。由于进行性MCI可能是旨在痴呆二级预防的临床试验的主要目标,这些患者应通过适当的生物标志物和神经影像学技术来识别。
