A Randomized Double-Blind Futility Clinical Trial of Creatine and Minocycline in Early Parkinson Disease

Authors

Bernard Ravina
Karl Kieburtz
Barbara Tilley
Kathleen Shannon
Caroline Tanner
G. Frederick Wooten
Brad Racette
Patricia Deppen
Richard B. Dewey
Brigid Hayward
Burton Scott
Joanne Field
Julie Carter
Matthew Brodsky
Pamela Andrews
Bala Manyam
Jacqueline Whetteckey
Jayaraman Rao
Holly A. Shill, Barrow Neurological InstituteFollow
et al.

Department

neurology

Document Type

Article

Abstract

Background: Creatine and minocycline were prioritized for testing in Phase II clinical trials based on a systematic evaluation of potentially disease modifying compounds for Parkinson disease (PD). Objective: To test whether creatine and minocycline alter the course of early PD relative to a predetermined futility threshold for progression of PD in a randomized, double-blind, Phase II futility clinical trial. Agents that do not perform better than the futility threshold are rejected as futile and are not considered for further study. Methods: Participants had a diagnosis of PD within 5 years, but did not require medications for the management of symptoms. The primary outcome was the change in the total Unified Parkinson€™s Disease Rating Scale (UPDRS) score from baseline to either the time when there was sufficient disability to warrant symptomatic therapy for PD or 12 months, whichever came first. Subjects were randomized 1:1:1 to receive creatine 10 g/day, minocycline 200 mg/day, or matching placebo. The futility threshold was set as a 30% reduction in UPDRS progression based on the placebo/tocopherol arm of the Deprenyl And Tocopherol Antioxidative Therapy Of Parkinsonism (DATATOP) trial. p Values ‰¤ 0.1 indicate futility. Results: Two hundred subjects were randomized to the three groups. Neither creatine (p = 0.96) nor minocycline (p = 0.66) could be rejected as futile based on the DATATOP futility threshold. The rate of progression for the calibration placebo group fell outside the 95% CI for the DATATOP historical control. In a sensitivity analysis, based on the threshold derived from the calibration placebo group, again neither drug could be rejected as futile. Tolerability was 91% in the creatine group and 77% in the minocycline group. Common adverse events included upper respiratory symptoms (26%), joint pain (19%), and nausea (17%). Conclusions: Both creatine and minocycline should be considered for definitive Phase III trials to determine if they alter the long term progression of Parkinson disease (PD). Additional factors must be weighed before selecting agents for Phase III trials, including safety, tolerability, activity, cost, and availability of these two agents in comparison with other agents currently in development for PD.

Medical Subject Headings

neurology

Publication Date

2006

Publication Title

Neurology

ISSN

0028-3878

Volume

66

Issue

5

First Page

664

Last Page

671

Digital Object Identifier (DOI)

10.1212/01.wnl.0000201252.57661.e1

Recommended Citation

Ravina, Bernard; Kieburtz, Karl; Tilley, Barbara; Shannon, Kathleen; Tanner, Caroline; Wooten, G. Frederick; Racette, Brad; Deppen, Patricia; Dewey, Richard B.; Hayward, Brigid; Scott, Burton; Field, Joanne; Carter, Julie; Brodsky, Matthew; Andrews, Pamela; Manyam, Bala; Whetteckey, Jacqueline; Rao, Jayaraman; Shill, Holly A.; and al., et, "A Randomized Double-Blind Futility Clinical Trial of Creatine and Minocycline in Early Parkinson Disease" (2006). Neurology. 241.
https://scholar.barrowneuro.org/neurology/241