Denise M. McHale scite author profile

We studied the temporal patterns of chorea and plasma levodopa profiles in 30 patients with Parkinson's disease whose motor fluctuations were difficult to characterize and treat on the basis of observation alone. We were able to determine whether chorea was associated with high levodopa concentrations or low levodopa concentrations or both. We found the following patterns of levodopa-associated chorea: chorea due to inadequate levodopa levels, chorea due to biphasic levodopa absorption, chorea associated with either rapid or slow levodopa absorption, and chorea due to long-duration levodopa absorption mimicking a sustained-release preparation. Seven patients benefited after their dosing schedules were rearranged as a result of information gained from monitoring. We conclude that any patient with levodopa-associated chorea who cannot be regulated on the basis of observation alone should be studied with simultaneous plasma levodopa measurements and clinical monitoring to detect an unusual plasma levodopa pattern that may be improved by adjustment of dosing schedule.

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Continuous levodopa infusions to treat complex dystonia in Parkinson's disease

Sage¹,

McHale²,

Sonsalla³

et al. 1989

Neurology

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We report the clinical spectrum of 3 patients with Parkinson's disease who experienced complex patterns of levodopa-related dystonia. Dystonia was unrelieved by multiple medication regimens but responded well to continuous, duodenal levodopa infusions. Patients were able to remain mobile without severe dystonia despite a very narrow window of benefit between the levodopa concentration necessary to achieve the "on" state and that which caused the onset of dystonic spasms.

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Persistent movement disorders induced by buspirone

LeWitt

Walters²,

Hening³

et al. 1993

Movement Disorders

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Buspirone, an azospirone compound, is a nonsedative anxiolytic that has achieved wide usage since its introduction in 1987. Although relatively free of side-effects, there have been several instances of dyskinesia and dystonia associated with the use of buspirone. We report two patients with persistent movement disorders that developed after prolonged treatment with the drug. One patient developed a lasting problem of cervical-cranial dystonia and tremors after treatment with buspirone at a dosage of 40 mg/day for several weeks. Another, receiving 30 mg/day for 6 weeks, experienced an exacerbation of preexisting spasmodic torticollis and tardive dyskinesia as well as the onset of involuntary phonations. As shown by these and other examples, buspirone poses the risk for inducing or exacerbating several types of movement disorders.

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A Blinded Study of the Suppressibility of Involuntary Movements in Huntingtonʼs Chorea, Tardive Dyskinesia, and L-DOPA-Induced Chorea

Walters¹,

McHale²,

Sage

et al. 1990

Clinical Neuropharmacology

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Denise M. McHale

The presence of free D-aspartic acid in rodents and man

Benefits of monitoring plasma levodopa in Parkinson's disease patients with drug‐induced chorea

Continuous levodopa infusions to treat complex dystonia in Parkinson's disease

Persistent movement disorders induced by buspirone

A Blinded Study of the Suppressibility of Involuntary Movements in Huntingtonʼs Chorea, Tardive Dyskinesia, and L-DOPA-Induced Chorea

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