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首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >Aphasic variant of Alzheimer disease: Clinical, anatomic, and genetic features
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Aphasic variant of Alzheimer disease: Clinical, anatomic, and genetic features

机译:阿尔茨海默病的失语症的变体:临床、解剖、遗传特性

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Objective:To identify features of primary progressive aphasia (PPA) associated with Alzheimer disease (AD) neuropathology. A related objective was to determine whether logopenic PPA is a clinical marker for AD.Methods:A total of 139 prospectively enrolled participants with a root diagnosis of PPA constituted the reference set. Those with autopsy or biomarker evidence of AD, and who had been evaluated at mild disease stages (Aphasia Quotient 85), were included (n = 19). All had quantitative language testing and APOE genotyping. Fifteen had MRI morphometry.Results:Impaired word-finding was the universal presenting complaint in the aphasic AD group. PPA clinical subtype was logopenic (n = 13) and agrammatic (n = 6). Fluency, repetition, naming, and grammaticality ranged from preserved to severely impaired. All had relative preservation of word comprehension. Eight of the 15 aphasic participants with AD showed no appreciable cortical atrophy at the individual level on MRI. As a group, atrophy was asymmetrically concentrated in the left perisylvian cortex. APOE epsilon 4 frequency was not elevated.Conclusions:There is a close, but not obligatory, association between logopenic PPA and AD. No language measure, with the possible exception of word comprehension, can confirm or exclude AD in PPA. Biomarkers are therefore essential for diagnosis. Asymmetry of cortical atrophy and normal APOE epsilon 4 prevalence constitute deviations from typical AD. These and additional neuropathologic features suggest that AD has biological subtypes, one of which causes PPA. Better appreciation of this fact should promote the inclusion of individuals with PPA and positive AD biomarkers into relevant clinical trials.
机译:目的:主要的识别特征进步的失语症(PPA)联系在一起阿尔茨海默病(AD)神经病理学。目标是确定logopenic PPA是一个临床的标志广告。139前瞻性的参与者根PPA构成的诊断参考集。广告,被评估在轻微的疾病阶段(85年失语商),包括(n =19)。APOE基因分型。形态测量学。通用的公元失语症患者的主诉组。13)和agrammatic (n = 6)。流利,重复,命名,语法性范围从保留严重受损。保存单词的理解。15失语症的参与者与广告没有显示明显的皮质萎缩在个体在MRI水平。不对称地集中在左边perisylvian皮层。不升高。不是必须的,logopenic PPA之间的联系和广告。除了单词的理解,可以证实或排除在PPA广告。诊断的必要条件。萎缩和正常APOEε4患病率构成偏离典型的广告。建议额外neuropathologic特性广告有生物学亚型,其中一个原因PPA。促进个人的包容和PPA积极的广告相关生物标志物在临床试用

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