Literature DB >> 19769916

Spastic hypertonia and movement disorders: pathophysiology, clinical presentation, and quantification.

Geoffrey Sheean1, John R McGuire.   

Abstract

A delayed consequence of a lesion affecting the upper motor neuron pathways is the appearance of some forms of motor overactivity, including spasticity. Many of these are caused by hyperexcitability of spinal reflexes, such as stretch reflexes (spasticity, tendon hyperreflexia) or flexor withdrawal reflexes (flexor spasms), and are elicited at rest by sensory stimulation. Spastic co-contraction is probably attributable to failure of reciprocal inhibition; it occurs only during active voluntary movement and constrains such movement. The basic underlying mechanism of these changes is not clear, although a change in the balance between the inhibitory and excitatory supraspinal upper motor neuron pathways toward net excitation most likely contributes. Increased intrinsic excitability of the alpha motor neurons is another possible factor. Spastic dystonia is most often seen as the presence of tonic muscle contraction in the absence of voluntary movement or spinal reflex activation, and the underlying mechanisms are obscure. Prolonged shortening of tissues, either because of weakness or muscle contraction, leads to stiffness of the soft tissues, which contributes to hypertonia and is thus self-perpetuating, and ultimately to contracture with fixed shortening. Some of these forms of motor overactivity produce involuntary movements (hyperkinetic), eg, flexor spasms, whereas others impair movement (hypokinetic), either voluntary movement, eg, spastic co-contraction, or passive movement, eg, spasticity. Quantification has mostly focused on hypertonia, that is, increased resistance at rest to passive movement. In the upper motor neuron syndrome, hypertonia could be caused by a combination of spasticity, spastic dystonia, and soft tissue stiffness (rheologic changes). Some measures, such as the Ashworth or Modified Ashworth Scales, quantify hypertonia but are very poor at distinguishing between spasticity and soft tissue stiffness. Another, the Tardieu Scale, is better at making this distinction, but quantification of the spasticity portion of hypertonia remains difficult, at least in a clinical setting.

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Year:  2009        PMID: 19769916     DOI: 10.1016/j.pmrj.2009.08.002

Source DB:  PubMed          Journal:  PM R        ISSN: 1934-1482            Impact factor:   2.298


  40 in total

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Review 2.  Emerging Therapies for Spastic Movement Disorders.

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3.  Optical inhibition of motor nerve and muscle activity in vivo.

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Journal:  Int Wound J       Date:  2019-03-20       Impact factor: 3.315

Review 5.  New perspectives on the development of muscle contractures following central motor lesions.

Authors:  J Pingel; E M Bartels; J B Nielsen
Journal:  J Physiol       Date:  2016-12-07       Impact factor: 5.182

6.  Activation and intermuscular coherence of distal arm muscles during proximal muscle contraction.

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Journal:  Exp Brain Res       Date:  2013-12-07       Impact factor: 1.972

7.  Left-Right Side-Specific Neuropeptide Mechanism Mediates Contralateral Responses to a Unilateral Brain Injury.

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Journal:  eNeuro       Date:  2021-05-25

8.  Monitoring Involuntary Muscle Activity in Acute Patients with Upper Motor Neuron Lesion by Wearable Sensors: A Feasibility Study.

Authors:  Andrea Merlo; Maria Giulia Montecchi; Francesco Lombardi; Xhejsi Vata; Aurora Musi; Mirco Lusuardi; Roberto Merletti; Isabella Campanini
Journal:  Sensors (Basel)       Date:  2021-04-30       Impact factor: 3.576

9.  Unilateral traumatic brain injury of the left and right hemisphere produces the left hindlimb response in rats.

Authors:  Georgy Bakalkin; Olga Nosova; Daniil Sarkisyan; Mathias Hallberg; Mengliang Zhang; Jens Schouenborg; Niklas Marklund; Hiroyuki Watanabe
Journal:  Exp Brain Res       Date:  2021-05-22       Impact factor: 1.972

10.  Elbow spasticity during passive stretch-reflex: clinical evaluation using a wearable sensor system.

Authors:  Chris A McGibbon; Andrew Sexton; Melony Jones; Colleen O'Connell
Journal:  J Neuroeng Rehabil       Date:  2013-06-19       Impact factor: 4.262

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