Pramipexole vs levodopa as initial treatment for Parkinson disease: a 4-year randomized controlled trial.

BACKGROUND The best way to initiate dopaminergic therapy for early Parkinson disease remains unclear. OBJECTIVE To compare initial treatment with pramipexole vs levodopa in early Parkinson disease, followed by levodopa supplementation, with respect to the development of dopaminergic motor complications, other adverse events, and functional and quality-of-life outcomes. DESIGN Multicenter, parallel-group, double-blind, randomized controlled trial. SETTING Academic movement disorders clinics at 22 sites in the United States and Canada. PATIENTS Patients with early Parkinson disease (N = 301) who required dopaminergic therapy to treat emerging disability, enrolled between October 1996 and August 1997 and observed until August 2001. INTERVENTION Subjects were randomly assigned to receive 0.5 mg of pramipexole 3 times per day with levodopa placebo (n = 151) or 25/100 mg of carbidopa/levodopa 3 times per day with pramipexole placebo (n = 150). Dosage was escalated during the first 10 weeks for patients with ongoing disability. Thereafter, investigators were permitted to add open-label levodopa or other antiparkinsonian medications to treat ongoing or emerging disability. MAIN OUTCOME MEASURES Time to the first occurrence of dopaminergic complications: wearing off, dyskinesias, on-off fluctuations, and freezing; changes in the Unified Parkinson's Disease Rating Scale and quality-of-life scales; and adverse events. RESULTS Initial pramipexole treatment resulted in a significant reduction in the risk of developing dyskinesias (24.5% vs 54%; hazard ratio, 0.37; 95% confidence interval [CI], 0.25-0.56; P<.001) and wearing off (47% vs 62.7%; hazard ratio, 0.68; 95% CI, 0.49-0.63; P =.02). Initial levodopa treatment resulted in a significant reduction in the risk of freezing (25.3% vs 37.1%; hazard ratio, 1.7; 95% CI, 1.11-2.59; P =.01). By 48 months, the occurrence of disabling dyskinesias was uncommon and did not significantly differ between the 2 groups. The mean improvement in the total Unified Parkinson's Disease Rating Scale score from baseline to 48 months was greater in the levodopa group than in the pramipexole group (2 +/- 15.4 points vs -3.2 +/- 17.3 points, P =.003). Somnolence (36% vs 21%, P =.005) and edema (42% vs 15%, P<.001) were more common in pramipexole-treated subjects than in levodopa-treated subjects. Mean changes in quality-of-life scores did not differ between the groups. CONCLUSIONS Initial treatment with pramipexole resulted in lower incidences of dyskinesias and wearing off compared with initial treatment with levodopa. Initial treatment with levodopa resulted in lower incidences of freezing, somnolence, and edema and provided for better symptomatic control, as measured by the Unified Parkinson's Disease Rating Scale, compared with initial treatment with pramipexole. Both options resulted in similar quality of life. Levodopa and pramipexole both appear to be reasonable options as initial dopaminergic therapy for Parkinson disease, but they are associated with different efficacy and adverse-effect profiles.

John Seibyl | Mark Stacy | Stanley Fahn | Rajesh Pahwa | Susan Bennett | Michel Panisset | Pamela Rainey | Karl Kieburtz | Roger Kurlan | Ira Shoulson | Anthony Lang | Joseph Jankovic | Arthur Watts | Blair Ford | J. Jankovic | W. Weiner | A. Lang | J. Seibyl | R. Pahwa | S. Fahn | J. Hubble | S. Factor | M. Mcdermott | K. Kieburtz | I. Shoulson | M. Stacy | C. Waters | K. Marek | D. Standaert | D. Fontaine | R. Holloway | P. Lewitt | R. Rodnitzky | E. Sime | B. Ford | A. Rajput | O. Suchowersky | R. Kurlan | M. Panisset | D. Riley | K. Biglan | C. Shults | J. Miyasaki | D. S. Russell | R. Pfeiffer | S. Wood | Kenneth Marek | J. Hammerstad | Cheryl Waters | Mickie Welsh | Robert G Holloway | Ronald Pfeiffer | Jean Hubble | Elspeth Sime | Janis Miyasaki | Oksana Suchowersky | B. Musch | Alicia Brocht | Peter LeWitt | M. Tennis | Tori Ross | Alicia F D Brocht | Cornelia L. Kamp | M. Welsh | A. Shinaman | L. Barclay | F. Wooten | F. Atassi | Giselle Petsinger | Leona D Borchert | A. Montgomery | L. Sutherland | C. Weeks | M. DeAngelis | C. Pantella | M. Harrigan | B. Fussell | S. Dillon | Barbara Alexander-Brown | P. Rainey | E. Rost-Ruffner | Diane L. Brown | S. Evans | Debra Berry | Jean Hall | T. Shirley | J. Dobson | B. Pfeiffer | Susan Bennett | S. Daigneault | K. Hodgeman | C. O'Connell | Karen Richard | A. Watts | Ali Rajput | Stewart Factor | Michael McDermott | William Weiner | Bruno Musch | Cornelia Kamp | Aileen Shinaman | Lynn Barclay | David S Russell | John Hammerstad | David Riley | David Standaert | Frederick Wooten | Farah Atassi | Robert Rodnitzky | Cliff Shults | Giselle Petsinger | Kevin Biglan | Leona Borchert | Amy Montgomery | Laura Sutherland | Carolyn Weeks | Maryan DeAngelis | Susan Wood | Carol Pantella | Mary Harrigan | Barbara Fussell | Sandra Dillon | Barbara Alexander-Brown | Marsha Tennis | Elke Rost-Ruffner | Diane Brown | Sharon Evans | Debra Berry | Jean Hall | Theresa Shirley | Judith Dobson | Deborah Fontaine | Brenda Pfeiffer | Susan Daigneault | Karen Hodgeman | Carolynn O'Connell | Tori Ross | Karen Richard | P. LeWitt | A. Brocht | D. Russell | E. Rost-ruffner

[1]  J. Kalbfleisch,et al.  The Statistical Analysis of Failure Time Data , 1980 .

[2]  John Seibyl,et al.  Pramipexole vs levodopa as initial treatment for Parkinson disease: A randomized controlled trial. Parkinson Study Group. , 2000, JAMA.

[3]  D. Calne,et al.  Assessment of Parkinson's Disease , 1984, Clinical neuropharmacology.

[4]  J H Ellenberg,et al.  Analysis of clinical trials by treatment actually received: is it really an option? , 1991, Statistics in medicine.

[5]  M. Hoehn,et al.  Parkinsonism , 1967, Neurology.

[6]  M Richards,et al.  Interrater reliability of the unified Parkinson's disease rating scale motor examination , 1994, Movement disorders : official journal of the Movement Disorder Society.

[7]  D. Brooks,et al.  A five-year study of the incidence of dyskinesia in patients with early Parkinson's disease who were treated with ropinirole or levodopa. , 2000, The New England journal of medicine.

[8]  W. Ondo,et al.  Clinical characteristics of pramipexole-induced peripheral edema. , 2000, Archives of neurology.

[9]  R Little,et al.  Intent-to-treat analysis for longitudinal studies with drop-outs. , 1996, Biometrics.

[10]  A. Williams EuroQol : a new facility for the measurement of health-related quality of life , 1990 .

[11]  M. Piercey,et al.  Functional Roles for Dopamine-Receptor Subtypes , 1995 .

[12]  A. Lang,et al.  Excessive daytime sleepiness and sudden-onset sleep in Parkinson disease: a survey by the Canadian Movement Disorders Group. , 2002, JAMA.