Rasagiline, Parkinson neuroprotection, and delayed-start trials
Still no satisfaction?
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Abstract
Rasagiline has been studied as a Parkinson disease (PD) neuroprotective agent in 2 major clinical trials, utilizing the delayed-start design in an attempt to separate symptomatic drug benefits from a disease-modifying effect. The ostensibly positive outcomes of these studies, however, are obscured by potential confounding factors that seem intrinsic to this trial design, including 1) very small changes in clinical outcome measures that could easily be overshadowed by other influences; 2) probable incomplete blinding to study end; 3) subjective components of the Unified Parkinson's Disease Rating Scale (UPDRS) scoring system; and 4) practice influences from repeated scoring. Interpretation of the recent Attenuation of Disease Progression with Azilect Given Once-daily (ADAGIO) trials is especially problematic given 1) divergent results with the 2 symptomatically beneficial doses and 2) variability in UPDRS scores with active rasagiline, which was twice the magnitude of the major finding of the study. These studies further illustrate the difficulty in documenting a disease-modifying effect when considering a PD drug with symptomatic benefit.
Glossary
- ADAGIO=
- Attenuation of Disease Progression with Azilect Given Once-daily trial;
- PD=
- Parkinson disease;
- TEMPO=
- TVP-1012 in Early Monotherapy for PD Outpatients study;
- UPDRS=
- Unified Parkinson's Disease Rating Scale.
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Letters: Rapid online correspondence
- Rasagiline, Parkinson neuroprotection, and delayed-start trials: Still no satisfaction?
- Erwin B. Montgomery Jr., University of Alabama at Birmingham, emontgom@uab.eduemontgom@uab.edu
Submitted July 07, 2010 - Rasagiline, Parkinson neuroprotection, and delayed-start trials: Still no satisfaction?
- Michael A. Schwarzchild, Massachusetts General Hospital, MassGeneral Inst. for Neurodegenerative Disease, 114 16th St, Boston, MA 02129michaels@helix.mgh.harvard.edu
- NONE
Submitted July 07, 2010 - Reply from the authors
- J. Eric Ahlskog, Mayo Clinic, Dept. of Neurology, Mayo Clinic, Rochester, Minnesota 55905eahlskog@mayo.edu
- Ryan J. Uitti (Jacksonville, FL; uitti@mayo.edu)
Submitted July 07, 2010
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