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痉挛的介绍和相关的小鼠模型。

Introduction to spasticity and related mouse models.

机构信息

University of Cologne, Faculty of Medicine, University Hospital Cologne, Department of Neurology, Cologne, Germany.

University of Cologne, Faculty of Medicine, University Hospital Cologne, Center of Neurosurgery, Cologne, Germany.

出版信息

Exp Neurol. 2021 Jan;335:113491. doi: 10.1016/j.expneurol.2020.113491. Epub 2020 Sep 29.

Abstract

Although spasticity is one of the most common causes of motor disability worldwide, its precise definition and pathophysiology remain elusive, which to date renders its experimental targeting tricky. At least in part, this difficulty is caused by heterogeneous phenotypes of spasticity-causing neurological disorders, all causing spasticity by involving upper motor neurons. The most common clinical symptoms are a series of rapid muscle contractions (clonus), an increased muscle tone (hypertonia), and augmented tendon reflex activity (hyperreflexia). This muscle overactivity is due to disturbed inhibition of spinal reflexes following upper motor neuron dysfunction. Despite a range of physical and pharmacological therapies ameliorating the symptoms, their targeted application remains difficult. Therefore, to date, spasticity impacts rehabilitative therapy, and no therapy exists that reverses the pathology completely. In contrast to the incidence and importance of spasticity, only very little pre-clinical work in animal models exists, and this research is focused on the cat or the rat spastic tail model to decipher altered reflexes and excitability of the motor neurons in the spinal cord. Meanwhile, the characterization of spasticity in clinically more relevant mouse models of neurological disorders, such as stroke, remains understudied. Here, we provide a brief introduction into the clinical knowledge and therapy of spasticity and an in-depth review of pre-clinical studies of spasticity in mice including the current experimental challenges for clinical translation.

摘要

虽然痉挛是全球最常见的运动障碍原因之一,但它的确切定义和病理生理学仍然难以捉摸,这使得其实验靶向治疗变得棘手。至少部分原因是引起痉挛性神经障碍的表型存在异质性,所有这些疾病都通过涉及上运动神经元引起痉挛。最常见的临床症状是一系列快速肌肉收缩(阵挛)、肌肉张力增加(高张力)和腱反射活动增强(反射亢进)。这种肌肉过度活跃是由于上运动神经元功能障碍后脊髓反射的抑制受到干扰。尽管有一系列物理和药理学疗法可以改善症状,但它们的靶向应用仍然很困难。因此,迄今为止,痉挛影响康复治疗,而且没有完全逆转病理的疗法。与痉挛的发病率和重要性相比,在动物模型中进行的临床前研究非常少,并且这项研究集中在痉挛性尾巴的猫或大鼠模型上,以解析脊髓运动神经元的改变反射和兴奋性。同时,中风等神经障碍更相关的临床小鼠模型中痉挛的特征仍然研究不足。在这里,我们简要介绍痉挛的临床知识和治疗方法,并深入回顾痉挛的临床前研究在小鼠中的应用,包括目前临床转化的实验挑战。

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