Selegiline to Zelapar Switch Study in Parkinson Disease Patients
NCT ID: NCT00640159
Last Updated: 2023-08-09
Study Results
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View full resultsBasic Information
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COMPLETED
PHASE4
48 participants
INTERVENTIONAL
2007-01-31
2008-08-31
Brief Summary
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Oral selegiline has low bio-availability and is typically dosed BID, for a total of 5-10 mg daily. Recently, the FDA approved a new orally disintegration tablet (ODT) formulation of selegiline, called ZelaparTM. This new formulation utilizes Zydis technology to dissolve in the mouth, with absorption through the oral mucosa, thereby largely bypassing the gut and avoiding first pass hepatic metabolism. This allows more active drug to be delivered at a lower dose. Consequently, Zelapar is dosed once-daily, up to 2.5 mg per day. There are no empirical data indicating whether the use of the new approved formulation of selegiline ODT (Zelapar) is superior or preferred by patients compared to traditional oral selegiline. It is believed that clinical efficacy will be preserved or enhanced, by delivering more active drug, with improved patient preference for the ODT formulation due to the once-daily dosing .
The effectiveness of orally disintegrating selegiline as an adjunct to carbidopa/levodopa in the treatment of PD was established in a multicenter randomized placebo-controlled trial (n=140; 94 received orally disintegrating selegiline, 46 received placebo) of three months' duration. Patients randomized to orally disintegrating selegiline received a daily dose of 1.25 mg for the first 6 weeks and a daily dose of 2.5 mg for the last 6 weeks. Patients were all treated with levodopa and could additionally have been on dopamine agonists, anticholinergics, amantadine, or any combination of these during the trial. At 12 weeks, orally disintegrating selegiline-treated patients had an average of 2.2 hours per day less "OFF" time compared to baseline. Placebo treated patients had 0.6 hours per day less "OFF" time compared to baseline. These differences were significant (p \< 0.001). Adverse events were very similar between drug and placebo.
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Detailed Description
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Inclusion Criteria:
1\. Idiopathic PD confirmed by at least two of the following signs: resting tremor, bradykinesia, rigidity 2. Male or female outpatients 3. Age 30-90 years 4. Current use of levodopa and oral selegiline (5-10 mg /day), stable for at least 1 month and well tolerated 5. Positive treatment response to current anti-parkinsonian medications in the opinion of the investigator 6. Acceptable contraception for females of child bearing potential 7. Willing and able to comply with study procedures. 8. Willing and able to give written informed consent prior to beginning any study procedures.
Exclusion Criteria:
1\. Atypical parkinsonism due to drugs, metabolic disorders, encephalitis, trauma, or other neurodegenerative diseases. 2. Significant cognitive or psychiatric impairment which, in the opinion of the investigator, would interfere with the ability to complete all the tests required in the protocol. 3. Participation in another clinical drug trial within the previous four weeks. 4. Patients on any medications contraindicated with Zelapar (including meperidine/Demerol, tramadol, methadone, propoxyphene, dextromethorphan, other selegiline products) 5. Patients with a known hypersensitivity to any formulation of selegiline or any of the inactive ingredients of Zelapar, or previous exposure to orally disintegrating selegiline 6. History of melanoma 7. Unstable/uncontrolled medical problems 8. History of drug/alcohol abuse 9. Patients currently taking rasagiline
The primary efficacy point is number of subjects who prefer Zydis selegiline vs. the number who prefer oral selegiline, or have no preference. Descriptive statistics will be used to present the percentages of persons and adverse event resolutions. The secondary endpoints will include changes in the UPDRS, PDQ-8, BDI, FSS, ESS, ratings of global improvement and change in dyskinesia from Baseline to the Day 40 visit. Appropriate parametric (t-tests) and non-parametric analyses (Wilcoxon signed rank comparisons) will be conducted based on the scale being analyzed. An intent to treat approach will be used in which all subjects receiving at least one dose of study medication will be included in the analyses.
Tolerability and efficacy of switching from oral selegiline to Zydis selegiline in patients with Parkinson's disease.
Conditions
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Study Design
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NA
SINGLE_GROUP
TREATMENT
NONE
Study Groups
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Selegiline
Open label switch from current oral selegiline dose to orally disintegrating selegiline (Zelapar) titrated to a dose of 2.5 mg QD.
Zelapar
Switch from oral selegiline to Zelapar 1.25 mg QD titrated to 2.5 mg QD
Interventions
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Zelapar
Switch from oral selegiline to Zelapar 1.25 mg QD titrated to 2.5 mg QD
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
2. Male or female outpatients
3. Age 30-90 years
4. Current use of levodopa and oral selegiline (5-10 mg /day), stable for at least 1 month and well tolerated
5. Positive treatment response to current anti-parkinsonian medications in the opinion of the investigator
6. Acceptable contraception for females of child bearing potential
7. Willing and able to comply with study procedures.
8. Willing and able to give written informed consent prior to beginning any study procedures.
Exclusion Criteria
2. Significant cognitive or psychiatric impairment which, in the opinion of the investigator, would interfere with the ability to complete all the tests required in the protocol.
3. Participation in another clinical drug trial within the previous four weeks.
4. Patients on any medications contraindicated with Zelapar (including meperidine/Demerol, tramadol, methadone, propoxyphene, dextromethorphan, other selegiline products)
5. Patients with a known hypersensitivity to any formulation of selegiline or any of the inactive ingredients of Zelapar, or previous exposure to orally disintegrating selegiline
6. History of melanoma
7. Unstable/uncontrolled medical problems
8. History of drug/alcohol abuse
9. Patients currently taking rasagiline
30 Years
90 Years
ALL
No
Sponsors
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Baylor College of Medicine
OTHER
Responsible Party
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Joseph Jankovic
Professor
Principal Investigators
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Greg Kricorian, MD
Role: STUDY_DIRECTOR
Valeant Pharmaceuticals
Locations
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Dee Silver, MD at Coastal Neurological Medical Group, Inc
La Jolla, California, United States
James Tetrud, MD at The Parkinson's Institute
Sunnyvale, California, United States
Stuart Isaacson, MD at Parkinson's Disease and Movement Disorder Center of Boca Raton
Boca Raton, Florida, United States
R. Malcolm Stewart, MD at Neurology Specialists of Dallas
Dallas, Texas, United States
PDCMDC 6550 Fannin, Suite 1801
Houston, Texas, United States
Countries
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References
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Ondo WG, Hunter C, Isaacson SH, Silver DE, Stewart RM, Tetrud JW, Davidson A. Tolerability and efficacy of switching from oral selegiline to Zydis selegiline in patients with Parkinson's disease. Parkinsonism Relat Disord. 2011 Feb;17(2):117-8. doi: 10.1016/j.parkreldis.2010.10.001. Epub 2010 Nov 16.
Other Identifiers
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H-20709
Identifier Type: -
Identifier Source: org_study_id
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