February 10 Highlight and Commentary

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February 10 Highlight and Commentary

Clozapine and dyskinesia in Parkinson disease

Durif et al. studied the effect of clozapine on levodopa-induceddyskinesias (LID) in 50 parkinsonian patients in a 10-week randomizedplacebo-controlled study. The duration of LID was reduced by2 hours and their intensities by 50%. The mean clozapine dosewas 40 mg. Three patients in the clozapine group developed hypereosinophilia,which resolved rapidly after stopping the drug.

see page 381

Progress in combating levodopa-induced dyskinesia

Commentary by Robert L. Rodnitzky, MD

Levodopa-induced dyskinesia (LID) is a source of motoric orsocial disability in a significant percentage of patients undergoingtreatment for Parkinson disease (PD). This complication appearsin approximately 40% of patients who have received levodopatherapy for 4 to 6 years.¹ In their mildest form LID may beapparent to family members, but not the patient. When more severe,these abnormal involuntary movements can impair gait and balance,interfere with ordinary activities of daily living such as feeding,or result in social withdrawal due to embarrassment. Patientswith moderate or severely advanced PD are most commonly affectedby this adverse effect, but patients with young onset PD ofany severity are prone to develop early and severe LID.

There has been some progress in treating this complication.Medical therapy with amantadine, an NMDA antagonist, and surgicaltherapies such as pallidotomy, pallidal stimulation, or subthalamicnucleus stimulation may help.² Still, many patients cannot tolerateor are not improved by the former treatment, and are not suitablecandidates for the latter.

There is clearly a need for additional effective therapies ofthis condition, and a host of potential approaches have beensuggested ranging from blockade of the adenosine A_2A or alpha2 adrenergic receptors, to treatment with 5HT1A serotonin agonists,to mention only a few. Durif et al. provide evidence, basedon a double-blind placebo-controlled study, that the atypicalantipsychotic agent clozapine effectively reduces the severityand duration of LID in PD patients. Whereas this result hasbeen suggested in previous open-label studies, the more rigorousdemonstration of clozapine’s antidyskinetic propertiesin this study is a welcome development. The exact mechanismby which clozapine improves LID is still unclear, mirroringour incomplete understanding of the physiochemical basis ofthis complication.

Whereas these data may appropriately lower the clinician’sthreshold to prescribe clozapine for the treatment of LID, theuse of this agent must still be balanced by awareness of itsrelatively high side effect profile, including the rare, butpotentially fatal, complication of agranulocytosis.³ However,as LID are potentially disabling for so many PD patients, thiscaveat should be considered a precaution, not a prohibitionfor the use of this otherwise useful medication.

see page 381

References

Ahlskog E, Muenter MD. Frequency of levodopa-related dyskinesias and motor fluctuations as estimated from the cumulative literature. Mov Disord. 2001; 16: 448–458.[Medline]
Krack P, Batir A, Van Blercom N, et al. Five-year follow-up of bilateral stimulation of the subthalamic nucleus in advanced Parkinson’s disease. N Engl J Med. 2003; 349: 1925–1934.[Abstract/Free Full Text]
Iqbal MM, Rahman AH, Husain Z, Mahmud SZ, Ryan W, Feldman JM. Clozapine: a clinical review of adverse effects and management. Ann Clin Psychiatry. 2003; 15: 33–48.[Medline]

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