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基于人群的老龄化纵向样本中痴呆症的病理相关性。

Pathological correlates of dementia in a longitudinal, population-based sample of aging.

作者信息

Sonnen Joshua A, Larson Eric B, Crane Paul K, Haneuse Sebastien, Li Ge, Schellenberg Gerald D, Craft Suzanne, Leverenz James B, Montine Thomas J

机构信息

Department of Pathology, University of Washington, Seattle, WA, USA.

出版信息

Ann Neurol. 2007 Oct;62(4):406-13. doi: 10.1002/ana.21208.

Abstract

OBJECTIVE

Previously published community- or population-based studies of brain aging and dementia with autopsy were restricted to a single sex, a single ethnic group, Roman Catholic clergy, or focused pathological assessments. Our goal was to determine the independent pathological correlates associated with dementia in a typical US population.

METHODS

We evaluated autopsy data from the Adult Changes in Thought study, an ongoing longitudinal, population-based study of brain aging and dementia. Analyses were based on data collected from about 3,400 people 65 years or older who were cognitively intact at the time of enrollment in the Group Health Cooperative in King County, Washington. All consecutive autopsies (n = 221; 20% of deaths) from this cohort were evaluated and analyzed by weighted multivariate analysis to account for potential participation bias.

RESULTS

After adjusting for age, sex, education, and APOE, independent correlates of dementia (relative risk, 95% confidence interval; overall p value) included Braak stage (V/VI vs 0/I/II: 5.89, 1.62-17.60; p < 0.05), number of cerebral microinfarcts in standardized sections (>2 vs none: 4.80, 1.91-10.26; p < 0.001), and neocortical Lewy bodies (any vs none: 5.08, 1.37-18.96; p < 0.05). Estimates of adjusted population attributable risk for these three processes were 45% for Braak stage, 33% for microinfarcts, and 10% for neocortical Lewy bodies.

INTERPRETATION

Our results underscore the therapeutic imperative for Alzheimer's and Lewy body diseases, and provide evidence to support the immediate use of strategies that target cerebral microinfarcts as a means to partially prevent or delay the onset of dementia.

摘要

目的

先前发表的基于社区或人群的脑老化与痴呆症尸检研究仅限于单一性别、单一族裔群体、罗马天主教神职人员,或侧重于病理评估。我们的目标是确定美国典型人群中与痴呆症相关的独立病理关联因素。

方法

我们评估了“成人思维变化研究”的尸检数据,这是一项正在进行的基于人群的脑老化与痴呆症纵向研究。分析基于从华盛顿州金县Group Health合作社登记时认知功能完好的约3400名65岁及以上人群收集的数据。对该队列中的所有连续尸检(n = 221;占死亡人数的20%)进行评估,并通过加权多变量分析进行分析,以考虑潜在的参与偏倚。

结果

在调整年龄、性别、教育程度和APOE后,痴呆症的独立关联因素(相对风险,95%置信区间;总体p值)包括Braak分期(V/VI期与0/I/II期:5.89,1.62 - 17.60;p < 0.05)、标准化切片中的脑微梗死数量(>2个与无:4.80,1.91 - 10.26;p < 0.001)以及新皮质路易体(有与无:5.08,1.37 - 18.96;p < 0.05)。这三个过程的调整后人群归因风险估计值分别为:Braak分期45%,微梗死33%,新皮质路易体10%。

解读

我们的结果强调了针对阿尔茨海默病和路易体病进行治疗的紧迫性,并提供证据支持立即采用针对脑微梗死的策略,作为部分预防或延迟痴呆症发作的一种手段。

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