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进行性失语和言语失用的临床病理及影像学关联

Clinicopathological and imaging correlates of progressive aphasia and apraxia of speech.

作者信息

Josephs Keith A, Duffy Joseph R, Strand Edyth A, Whitwell Jennifer L, Layton Kenneth F, Parisi Joseph E, Hauser Mary F, Witte Robert J, Boeve Bradley F, Knopman David S, Dickson Dennis W, Jack Clifford R, Petersen Ronald C

机构信息

Department of Neurology, Division of Movement Disorders and Behavioral Neurology, Mayo Clinic, Rochester, MN 55905,

出版信息

Brain. 2006 Jun;129(Pt 6):1385-98. doi: 10.1093/brain/awl078. Epub 2006 Apr 13.

Abstract

Apraxia of speech (AOS) is a motor speech disorder characterized by slow speaking rate, abnormal prosody and distorted sound substitutions, additions, repetitions and prolongations, sometimes accompanied by groping, and trial and error articulatory movements. Although AOS is frequently subsumed under the heading of aphasia, and indeed most often co-occurs with aphasia, it can be the predominant or even the sole manifestation of a degenerative neurological disease. In this study we determine whether the clinical classifications of aphasia and AOS correlated with pathological diagnoses and specific biochemical and anatomical structural abnormalities. Seventeen cases with initial diagnoses of a degenerative aphasia or AOS were re-classified independently by two speech-language pathologists--blinded to pathological and biochemical findings--into one of five operationally defined categories of aphasia and AOS. Pathological diagnoses in the 17 cases were progressive supranuclear palsy in 6, corticobasal degeneration in 5, frontotemporal lobar degeneration with ubiquitin-only-immunoreactive changes in 5 and Pick's disease in 1. Magnetic resonance imaging analysis using voxel-based morphometry (VBM), and single photon emission tomography were completed, blinded to the clinical diagnoses, and clinicoimaging and clinicopathological associations were then sought. Interjudge clinical classification reliability was 87% (kappa = 0.8) for all evaluations. Eleven cases had evidence of AOS, of which all (100%) had a pathological diagnosis characterized by underlying tau biochemistry, while five of the other six cases without AOS did not have tau biochemistry (P = 0.001). A majority of the 17 cases had more than one yearly evaluation, demonstrating the evolution of the speech and language syndromes, as well as motor signs. VBM revealed the premotor and supplemental motor cortices to be the main cortical regions associated with AOS, while the anterior peri-sylvian region was associated with non-fluent aphasia. Refining the classification of the degenerative aphasias and AOS may be necessary to improve our understanding of the relationships among behavioural, pathological and imaging correlations.

摘要

言语失用症(AOS)是一种运动性言语障碍,其特征为语速缓慢、韵律异常以及声音替代、添加、重复和延长失真,有时伴有摸索动作和试错性发音动作。尽管AOS常被归入失语症范畴,且实际上最常与失语症同时出现,但它也可能是退行性神经疾病的主要甚至唯一表现形式。在本研究中,我们确定失语症和AOS的临床分类是否与病理诊断以及特定的生化和解剖结构异常相关。17例最初诊断为退行性失语症或AOS的病例由两名言语病理学家独立重新分类——对病理和生化结果不知情——分为失语症和AOS的五个操作性定义类别之一。17例病例的病理诊断为:6例进行性核上性麻痹,5例皮质基底节变性,5例额颞叶变性伴仅泛素免疫反应性改变,1例匹克病。在对临床诊断不知情的情况下完成了基于体素的形态测量(VBM)磁共振成像分析和单光子发射断层扫描,然后寻找临床影像学和临床病理关联。所有评估的评判者间临床分类可靠性为87%(kappa = 0.8)。11例有AOS证据,其中所有病例(100%)的病理诊断以潜在的tau生物化学为特征,而其他6例无AOS的病例中有5例没有tau生物化学(P = 0.001)。17例中的大多数病例接受了不止一次年度评估,显示了言语和语言综合征以及运动体征的演变。VBM显示运动前区和辅助运动皮层是与AOS相关的主要皮质区域,而颞叶周围前部区域与非流畅性失语症相关。可能有必要完善退行性失语症和AOS的分类,以增进我们对行为、病理和影像学关联之间关系的理解。

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