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Spasticity

Last updated: December 1, 2022

Summarytoggle arrow icon

Spasticity is defined as a velocity-dependent increase in muscle tone that manifests with resistance to movement and involuntary muscle spasms and contractions. It is caused by a lesion in the descending motor pathways. Common etiologies of spasticity include multiple sclerosis, stroke, tumor, cerebral palsy, and spinal or peripheral nerve injury. Nerve conduction studies and imaging of the brain and/or spinal cord may be requested to determine the underlying etiology. The management of spasticity is broad and may include physical and occupational therapy, pharmacotherapy (i.e., muscle relaxants such as diazepam, tizanidine, baclofen, or dantrolene; paralytics such as botulinum toxin), or surgery.

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Pathophysiologytoggle arrow icon

  • The mechanism of spasticity is not completely understood.
  • It is thought that upper motor neuron damage leads to loss of descending inhibitory inputs → increased muscle stretch reflex → increased muscle tone

References:[1]

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Clinical featurestoggle arrow icon

  • Increased muscle tone and velocity-dependent resistance to movement
    • Elicited by flexion and extension of various muscles with alternating speed
    • Clasp knife phenomenon: initial resistance (“catch”) when a limb is moved rapidly, followed by a sudden decrease in resistance; observed in patients with upper motor neuron lesions
    • Upper extremity flexors and lower extremity extensors are usually more affected.
    • Must be distinguished from rigidity
  • Involuntary muscle spasms or contractions

References:[1]

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Diagnosistoggle arrow icon

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Treatmenttoggle arrow icon

  • Physiotherapy: including splinting of the affected extremity
  • Medical therapy: The most commonly used medication is baclofen; however, a variety of treatments (single and/or in combination) may be used and depend on patient-specific factors and patient response.
Overview of oral muscle relaxants
Drug Mechanism of action Indication Side effects
Baclofen
  • Agonism at GABAB receptor in the spinal cord
  • Can also be intrathecally administered
Dantrolene
Cyclobenzaprine
  • Muscle spasticity

Oral α2 adrenergic agonists

(e.g., tizanidine, clonidine)

Oral benzodiazepines

(e.g., diazepam, clonazepam)

  • Indirect GABAA agonism by increasing the opening frequency of Cl- channels → ↑ GABAAaction
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Complicationstoggle arrow icon

  • Musculoskeletal deformity
  • Impaired mobility
  • Reduced functional independence
  • Pain

We list the most important complications. The selection is not exhaustive.

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Prognosistoggle arrow icon

The prognosis of spasticity depends on the underlying condition.

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