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额颞叶痴呆的诊断与病程

The diagnosis and course of frontotemporal dementia.

作者信息

Kertesz Andrew, Blair Mervin, McMonagle Paul, Munoz David G

机构信息

Cognitive Neurology, St Joseph's Hospital, London, and Department of Pathology, University of Western Ontario, Canada.

出版信息

Alzheimer Dis Assoc Disord. 2007 Apr-Jun;21(2):155-63. doi: 10.1097/WAD.0b013e31806547eb.

Abstract

The course of frontotemporal dementia (FTD) is examined in a prospective, incipient clinical cohort. Three hundred nineteen patients were followed yearly for an average of 3.6 years. The relative frequencies at presentation were Behavioral variety (FTD-bv) 37.6%, Primary Progressive Aphasia (PPA) 31.6%, possible PPA 10.6%, Corticobasal Syndrome (CBDS) and Progressive Supranuclear Palsy (PSP) 8.1%, Semantic Dementia (SD) 6.6%, and possible FTD 5.3%. The age of onset was significantly lower in the FTD-bv and SD groups than in the rest, but survival and sex distribution was similar in all groups. The evolution is characterized by the appearance of additional FTD syndromes in two-thirds of the patients. A significant association of SD with FTD-bv and CBDS/PSP with PPA was found. The Frontal Behavioral Inventory was highly sensitive and specific for FTD-bv. Visuospatial function was preserved except in CBDS/PSP. The clinical diagnosis showed a positive predictive value of 87% against autopsy in 67 patients. Multiple syndromes increase the likelihood of FTD pathology. In conclusion, the clinical associations follow the tau-negative and tau-positive pathologic dichotomy to some extent, but there is too much overlap to consider the clinical groups or their associations separate diseases.

摘要

在一个前瞻性的早期临床队列中对额颞叶痴呆(FTD)的病程进行了研究。319名患者每年接受随访,平均随访3.6年。就诊时各类型的相对频率分别为:行为变异型(FTD-bv)37.6%,原发性进行性失语(PPA)31.6%,可能的PPA 10.6%,皮质基底节综合征(CBDS)和进行性核上性麻痹(PSP)8.1%,语义性痴呆(SD)6.6%,以及可能的FTD 5.3%。FTD-bv组和SD组的发病年龄显著低于其他组,但所有组的生存率和性别分布相似。疾病进展的特点是三分之二的患者出现了额外的FTD综合征。发现SD与FTD-bv之间以及CBDS/PSP与PPA之间存在显著关联。额叶行为量表对FTD-bv具有高度敏感性和特异性。除CBDS/PSP外,视觉空间功能均得以保留。在67例患者中,临床诊断相对于尸检的阳性预测值为87%。多种综合征增加了FTD病理改变的可能性。总之,临床关联在一定程度上遵循tau阴性和tau阳性病理二分法,但存在过多重叠,不能将临床组或它们的关联视为独立的疾病。

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