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[肌萎缩侧索硬化症的表型变异]

[Phenotypic variation in ALS].

作者信息

Sasaki Shoichi

机构信息

Department of Neurology, Neurological Institute, Tokyo Women's Medical University.

出版信息

Rinsho Shinkeigaku. 2006 Nov;46(11):825-7.

Abstract

Making a diagnosis of typical amyotrophic lateral sclerosis (ALS) is not a tough job, but when it comes to atypical forms of motor neuron disease (MND) which are not uncommon in clinical setting, we may have some difficulty to diagnose ALS/MND. There is striking phenotypic variation in sporadic ALS/MND, such as frail arm syndrome (brachial amyotrophic diplegia), pseudopolyneuritic form, hemiplegic type, ALS/MND with markedly extended involvement beyond the motor system, and MND with basophilic inclusion bodies. These variations must be recognized if physicians are to tailor advice on disease progression, prognosis, drug therapy, and care to the needs of the individual. Clinical trials of new therapeutic agents have been performed, on the assumption that patients with ALS/MND have the same underlying etiology, addressing the heterogeneous population of the patients under a single diagnostic category. This can be detrimental to the well-being of the individual, because clinical heterogeneity may mask drug effects in clinical trials. The attempt to categorize subgroups based on the clinical and pathological backgrounds within the spectrum of ALS/MND may be a critical step in facilitating clinical research in ALS/MND. Definition of clinicopathologic syndromes in patients with ALS/MND is an important challenging task that cannot be ignored.

摘要

做出典型肌萎缩侧索硬化症(ALS)的诊断并非难事,但对于临床中并不罕见的非典型运动神经元病(MND)形式,我们在诊断ALS/MND时可能会遇到一些困难。散发性ALS/MND存在显著的表型变异,如虚弱手臂综合征(臂丛性肌萎缩性双侧瘫)、假多神经炎型、偏瘫型、累及范围明显超出运动系统的ALS/MND以及伴有嗜碱性包涵体的MND。如果医生要根据个体需求提供关于疾病进展、预后、药物治疗和护理的建议,就必须认识到这些变异。新治疗药物的临床试验是在假设ALS/MND患者具有相同潜在病因的前提下进行的,将不同类型的患者归为单一诊断类别。这可能对个体健康有害,因为临床异质性可能会在临床试验中掩盖药物效果。根据ALS/MND范围内的临床和病理背景对亚组进行分类的尝试,可能是促进ALS/MND临床研究的关键一步。定义ALS/MND患者的临床病理综合征是一项重要且不可忽视的具有挑战性的任务。

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