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肌萎缩侧索硬化症的运动表型异质性、局灶性和扩散:解析运动神经元变性

ALS motor phenotype heterogeneity, focality, and spread: deconstructing motor neuron degeneration.

作者信息

Ravits John M, La Spada Albert R

机构信息

Section of Neurology, Virginia Mason Medical Center, Seattle, WA, USA.

出版信息

Neurology. 2009 Sep 8;73(10):805-11. doi: 10.1212/WNL.0b013e3181b6bbbd.

Abstract

Heterogeneity of motor phenotypes is a clinically well-recognized fundamental aspect of amyotrophic lateral sclerosis (ALS) and is determined by variability of 3 independent primary attributes: body region of onset; relative mix of upper motor neuron (UMN) and lower motor neuron (LMN) deficits; and rate of progression. Motor phenotypes are determined by the anatomy of the underlying neuropathology and the common defining elements underlying their heterogeneity are that motor neuron degeneration is fundamentally a focal process and that it spreads contiguously through the 3-dimensional anatomy of the UMN and LMN levels, thus causing seemingly complex and varied clinical manifestations. This suggests motor neuron degeneration in ALS is in actuality a very orderly and actively propagating process and that fundamental molecular mechanisms may be uniform and their chief properties deduced. This also suggests opportunities for translational research to seek pathobiology directly in the less affected regions of the nervous system.

摘要

运动表型的异质性是肌萎缩侧索硬化症(ALS)临床上公认的一个基本特征,它由3个独立的主要属性的变异性决定:发病的身体部位;上运动神经元(UMN)和下运动神经元(LMN)缺陷的相对组合;以及进展速度。运动表型由潜在神经病理学的解剖结构决定,其异质性的共同定义要素是运动神经元变性从根本上说是一个局灶性过程,并且它通过UMN和LMN水平的三维解剖结构连续扩散,从而导致看似复杂多样的临床表现。这表明ALS中的运动神经元变性实际上是一个非常有序且积极传播的过程,并且基本分子机制可能是统一的,其主要特性可以推导出来。这也为转化研究提供了机会,以便直接在神经系统受影响较小的区域寻找病理生物学。

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