Bürk K, Stevanin G, Didierjean O, Cancel G, Trottier Y, Skalej M, Abele M, Brice A, Dichgans J, Klockgether T
Department of Neurology, University of Tübingen, Germany.
J Neurol. 1997 Apr;244(4):256-61. doi: 10.1007/s004150050081.
The detailed clinical, electrophysiological and imaging data of three German autosomal dominant cerebellar ataxia (ADCA) families are reported. Linkage to SCA2 was established using microsatellite markers D12S105, D12S1339(1328), D12S1304(1329) yielding a lod score exceeding +3.0 for the combined data. Analysis of the pedigree data provided evidence of anticipation as observed in other neurodegenerative disorders due to polyglutamine expansion encoded by a CAG repeat. This hypothesis was confirmed by the detection of the SCA2-specific pathological protein using the 1C2 monoclonal antibody which selectively recognizes large polyglutamine expansions and the characterization of a CAG expansion in the patients. Clinically, the families were characterized by progressive ataxia of stance, gait and limbs. Saccade velocity was markedly reduced in SCA2. Further oculomotor findings were gaze palsy, impaired smooth pursuit and reduced optokinetic reflex. Dementia and pyramidal tract signs were rather rare, while peripheral involvement (reduced or absent ankle reflexes, fasciculation-like movements, amyotrophy) was a prominent feature. Electrophysiological investigations provided evidence of sensory neuropathy of the axonal type and degeneration of the posterior columns. Imaging studies demonstrated severe shrinkage of brain-stem structures even in early stages of the disease.
报道了三个德国常染色体显性遗传性小脑共济失调(ADCA)家系的详细临床、电生理和影像学数据。利用微卫星标记D12S105、D12S1339(1328)、D12S1304(1329)确定了与SCA2的连锁关系,合并数据的对数优势比分超过+3.0。系谱数据分析提供了早现的证据,这在其他由CAG重复序列编码的多聚谷氨酰胺扩增导致的神经退行性疾病中也有观察到。使用1C2单克隆抗体检测SCA2特异性病理蛋白,该抗体可选择性识别大的多聚谷氨酰胺扩增,并对患者的CAG扩增进行特征分析,从而证实了这一假说。临床上,这些家系的特征为姿势、步态和肢体的进行性共济失调。SCA2患者的扫视速度明显降低。进一步的动眼神经检查发现有凝视麻痹、平稳跟踪受损和视动反射减弱。痴呆和锥体束征相当少见,而周围神经受累(踝反射减弱或消失、束颤样运动、肌萎缩)是一个突出特征。电生理检查提供了轴索性感觉神经病变和后索变性的证据。影像学研究表明,即使在疾病早期,脑干结构也会严重萎缩。
