Periodic Limb Movement Disorder

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Background

Periodic limb movement disorder (PLMD) is unique in that the movements occur during sleep. Most other movement disorders manifest during wakefulness. The condition is remarkably periodic, and the movements may cause poor sleep and subsequent daytime somnolence. PLMD may occur with other sleep disorders and is related to, but not synonymous with, restless legs syndrome (RLS), a less specific condition with sensory features that manifest during wakefulness. The majority of patients with RLS have PLMD, but the reverse is not true. Treatment involves either dopaminergic medication in an attempt to modify activity of the subcortical motor system or, more commonly, sedative medications to allow uninterrupted sleep. Many new agents are proving efficacious for treatment as well.

Etiology

The etiology of the primary form of periodic limb movement disorder is uncertain. Suprasegmental disinhibition of the descending inhibitory pathways may be a factor. Vetrugno and colleagues report that evidence supports neuronal hyperexcitability with involvement of the central pattern generator for gait as the pathophysiology of periodic limb movement.[1] This results in decreased dopamine transmission, potentially supporting the use of dopaminergic therapy to treat the condition.

Because the etiology is not clear, treatment is primarily to treat symptoms and does not modify the disease. Studies differ regarding the frequency of polyneuropathy in cases of periodic limb movement disorder. Martinez-Mena and Pastor found that only 1 of 9 patients had signs of neuropathy.[2]

The secondary forms of periodic limb movement disorder may be due to diabetes mellitus, spinal cord tumor, sleep apnea syndrome, narcolepsy, uremia, or anemia.[3] Many authors report an association between attention deficit hyperactivity disorder (ADHD) and periodic limb movement disorder. Antidopaminergic, dopaminergic, or tricyclic drug therapy or cessation of treatment with barbiturates or benzodiazepines may initiate the syndrome as well.[4] Voderholzer and colleagues noted an increased incidence of periodic limb movements during sleep in patients with Gilles de la Tourette syndrome.[5] However, the authors emphasized that the different responses to pharmacological treatments are evidence against a pathophysiological relationship between periodic limb movement disorder and Gilles de la Tourette syndrome.

Potential risk factors or etiologic factors for secondary periodic limb movement disorder include the following:

Epidemiology

The prevalence of periodic leg movements in sleep (PLMS) is estimated to be 4–11% in adults.[6] PLMS are most frequently a symptom of restless legs syndrome (RLS).They also often occur in narcolepsy, sleep apnea syndrome, and REM sleep behavior disorder. Some patients with otherwise unexplained insomnia or excessive daytime sleepiness exhibit an elevated number of PLMS, a condition defined as periodic limb movement disorder (PLMD).

Prognosis

The idiopathic form of this syndrome may be chronic. Relapses and remissions may occur, but treatment does not appear to modify the disease.

The secondary form of this syndrome may cease with treatment of the underlying cause.

Complications

Picchietti and colleagues suggested that the sleep disruption in periodic limb movement disorder could contribute to the inattention and hyperactivity of some children who have ADHD.[7]

Some research suggests that periodic limb movements with arousals are associated with subsequent nonsustained ventricular tachycardia (NSVT). The study of older men in their 70s and 80s found that periodic limb movements during sleep with arousal was associated with a threefold increased risk for NSVT shortly after the episode.[8]

Patient Education

Informing the bed partner of the condition is important so that potentially negative physical contact may be explained on a neurological (rather than an intentional) basis.

For excellent patient education resources, visit eMedicineHealth's Sleep Disorders Center. Also, see eMedicineHealth's patient education articles Periodic Limb Movement Disorder, Restless Legs Syndrome, Sleep Disorders in Women, and Sleep Disorders and Aging.

History

Periodic limb movement disorder (PLMD) is characterized by periodic episodes of repetitive limb movements during sleep, which most often occur in the lower extremities. These movements may cause awakening during the night resulting in excessive daytime sleepiness. Often, the presenting complaint is poor sleep or unexplained insomnia and daytime somnolence.[9] Researchers report that sleep changes induced by periodic limb movements during sleep are associated with decreased physical and psychological fitness on awakening.[10]

Leg movements associated with PLMD are stereotyped and involve one or both limbs. The movement simulates triple flexion with leg flexion, ankle dorsiflexion, and great toe extension; it lasts approximately 2 seconds and thus is not consistent with the rapid jerk that defines true myoclonus. The periodicity ranges from 20-40 seconds with a variable duration. The movements are said to occur mainly in non–rapid eye movement (REM) sleep.

Occasionally, a bed partner may provide the history of limb movements.

Nozawa and colleagues studied arousal index and movement index in periodic limb movement disorder and noted that the sleep-wake disorders associated with periodic limb movement relate to threshold of awakening.[11]

Growing evidence suggests a link between restless legs syndrome and periodic limb movement or sleep disorder. Picchietti et al provide evidence supporting the concept that periodic limb movement disorder may be a marker for an RLS genotype.[12]

The patient history may include ADHD. Walters et al provide an association between ADHD and sleep movement disorders including periodic limb movement disorder.[13]

Laboratory Studies

Because anemia, uremia, and the use of tricyclic antidepressant, antidopaminergic, or dopaminergic medications can lead to a secondary form of periodic limb movement disorder, laboratory screening studies should be obtained to rule out anemia or significant metabolic abnormalities.

A urine drug screen may be appropriate.

Sleep Study

Definitive diagnosis of periodic limb movement disorder (PLMD) requires polysomnography.[14] Observation in a sleep laboratory allows documentation of the movements and rapid diagnosis.

Periodic leg movements in sleep (PLMS) are a common symptom in restless legs syndrome and are a frequent finding in polysomnography. An elevated number of PLMS are defined as PLMD.

Variability from night to night occurs in both adults and children with documented PLMD.[15]

 

Other Tests

The Stanford PLM automatic detector (S-PLMAD) is a robust, automated leg movement detector used to score PLM functions. According to one study, the S-PLMAD works well in controls and sleep disorder patients.[16]

Approach Considerations

A 2012 update of treatment guidelines from the American Academy of Sleep Medicine indicate that although there are no studies of dopaminergic medication effects on periodic limb movement disorder (PLMD), many of the studies of dopaminergic medication effects on restless legs syndrome looked at periodic limb movements of sleep.[17]

Pharmacologic Therapy

According to the American Academy of Sleep Medicine practice parameters, the dopaminergic agents pramixpexole, ropinorole, rotigotine, and the combination of carbidopa/levodopa/entacapone, were shown in some studies to decrease periodic limb movement indices. Gabepentin and pregabalin also showed benefit in studies of subjects with restless legs syndrome.[17]

Nonpharmacologic Therapy

Some evidence shows that exercise therapy and cognitive-behavioral psychological intervention may provide benefit.[18]

Klassen et al report improvement with deep brain stimulation in Parkinson patients with PLMD.[19]

Medication Summary

Therapy does not modify the disease but does relieve symptoms. The arsenal of medication options is expanding and includes dopaminergic medications,[20, 21, 22] antiepileptic agents, and even opioids, although the controlled substances may not be appropriate first-line agents. Because most studies focused on restless legs syndrome, a similar and related (but separate) disorder, the best treatments for periodic limb movement are not known. However, using restless legs syndrome guidelines, dopaminergic agents are first-line treatment.

Clonazepam (Klonopin)

Clinical Context:  Useful in suppressing muscle contractions by facilitating action of GABA and other inhibitory neurotransmitters.

Class Summary

The efficacy of clonazepam in reducing the total number of periodic limb movements per hour has been reported.[23, 24]

Ropinirole (Requip, Requip XL)

Clinical Context:  Second-generation, nonergoline dopamine agonist that directly stimulates dopamine receptors in the brain. Possesses high specificity for D3 receptor subtype. Indicated for moderate-to-severe restless legs syndrome.

Pramipexole (Mirapex, Mirapex ER)

Clinical Context:  D2 and D3 receptor agonist recently approved by FDA for treating Parkinson disease; also used effectively in patients with restless legs syndrome.

Carbidopa/levodopa (Sinemet)

Clinical Context:  Large neutral amino acid absorbed in proximal small intestine by saturable carrier-mediated transport system. Absorption decreased by meals, which include other large neutral amino acids. However, only patients with meaningful motor fluctuations need consider low-protein or protein-redistributed diet. Greater consistency of absorption achieved when levodopa taken > 1 h after meals. Nausea often reduced if taken immediately following meals. Some patients with nausea benefit from additional carbidopa up to 200 mg/d.

Half-life approximately 2 h.

Most common acute adverse effects are nausea, hypotension, and hallucinations. Long-term adverse effects include motor fluctuations and dyskinesia (chorea).

Pergolide (Permax)

Clinical Context:  Pergolide was withdrawn from the US market March 29, 2007, because of heart valve damage resulting in cardiac valve regurgitation. It is important not to abruptly stop pergolide. Health care professionals should assess patients' need for dopamine agonist (DA) therapy and consider alternative treatment. If continued treatment with a DA is needed, another DA should be substituted for pergolide. For more information, see FDA MedWatch Product Safety Alert and Medscape Alerts: Pergolide Withdrawn From US Market.

Studies in patients with secondary PLM disorder caused by uremia revealed subjective improvement in sleep quality and objective reduction in limb movements during first hour of sleep; however, no objective improvement in sleep architecture was observed.

Class Summary

The levodopa/carbidopa combination has been considered an effective treatment for this condition in specific patients; on the other hand, some studies suggest that the medication may be the etiology of secondary periodic limb movement disorder in other patients. Pieta and colleagues studied pergolide in patients with secondary periodic limb movement disorder caused by uremia and found subjective improvement in sleep quality and objective reduction in limb movements during the first hour of sleep; however, no objective improvement in sleep architecture was observed.[25]

Gabapentin (Neurontin)

Clinical Context:  Mechanism of action uncertain; although has GABA-like structure, action at GABA receptors not shown clearly. Fortunately, considered relatively safe and thus may be considered for PLM disorder.

Class Summary

These agents are useful in managing severe muscle spasms.

Baclofen (Lioresal)

Clinical Context:  GABA agonist at slower potassium channels in cerebellum and spinal cord. May have efficacy in PLM disorder. Because works in spinal cord and less in brain cortex, calls into question neurologic origin of PLM.

Tiagabine (Gabitril)

Clinical Context:  Antiepileptic agent FDA approved for adjunctive treatment of certain seizure types. Recent evidence supports use in PLM disorder possibly because of GABA enhancing activity or because of improved sleep quality. FDA approved for seizures at doses up to 56 mg/d. Evidence suggests that use for PLM disorder requires far lower doses, possibly 4-8 mg at bedtime.

Class Summary

These agents exert their effects by inhibiting release of excitatory neurotransmitters.

What is periodic limb movement disorder (PLMD)?What causes periodic limb movement disorder (PLMD)?What are the risk factors for secondary periodic limb movement disorder (PLMD)?What is the prevalence of periodic limb movement disorder (PLMD)?What is the prognosis of periodic limb movement disorder (PLMD)?What are the possible complications of periodic limb movement disorder (PLMD)?What is included in patient education about periodic limb movement disorder (PLMD)?Which clinical history findings are characteristic of periodic limb movement disorder (PLMD)?What are the differential diagnoses for Periodic Limb Movement Disorder?What is the role of lab testing in the workup of periodic limb movement disorder (PLMD)?What is the role of a sleep study in the workup of periodic limb movement disorder (PLMD)?What is the role of the Stanford PLM automatic detector (S-PLMAD) in the workup of periodic limb movement disorder (PLMD)?Which organization has released guidelines on the treatment of periodic limb movement disorder (PLMD)?What is the role of medications in the treatment of periodic limb movement disorder (PLMD)?What are the nonpharmacologic treatments for periodic limb movement disorder (PLMD)?Which medications are used in the treatment of periodic limb movement disorder (PLMD)?Which medications in the drug class Skeletal muscle relaxants are used in the treatment of Periodic Limb Movement Disorder?Which medications in the drug class Anticonvulsants are used in the treatment of Periodic Limb Movement Disorder?Which medications in the drug class Dopaminergic agents are used in the treatment of Periodic Limb Movement Disorder?Which medications in the drug class Benzodiazepines are used in the treatment of Periodic Limb Movement Disorder?

Author

Wayne E Anderson, DO, FAHS, FAAN, Assistant Professor of Internal Medicine/Neurology, College of Osteopathic Medicine of the Pacific Western University of Health Sciences; Clinical Faculty in Family Medicine, Touro University College of Osteopathic Medicine; Clinical Instructor, Departments of Neurology and Pain Management, California Pacific Medical Center

Disclosure: Nothing to disclose.

Specialty Editors

Francisco Talavera, PharmD, PhD, Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Received salary from Medscape for employment. for: Medscape.

Chief Editor

Selim R Benbadis, MD, Professor, Director of Comprehensive Epilepsy Program, Departments of Neurology and Neurosurgery, Tampa General Hospital, University of South Florida Morsani College of Medicine

Disclosure: Serve(d) as a director, officer, partner, employee, advisor, consultant or trustee for: Ceribell, Eisai, Greenwich, Growhealthy, LivaNova, Neuropace, SK biopharmaceuticals, Sunovion<br/>Serve(d) as a speaker or a member of a speakers bureau for: Eisai, Greenwich, LivaNova, Sunovion<br/>Received research grant from: Cavion, LivaNova, Greenwich, Sunovion, SK biopharmaceuticals, Takeda, UCB.

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