A randomized, double-blind, placebo-controlled study of latrepirdine in patients with mild to moderate Huntington disease.

Karl K Kieburtz,Gb Landwehrmeyer,Merit Cudkowicz,E.R. Dorsey,Andrew Feigin,Victoria Hunt,Elise Kayson,Michael P. McDermott,S Noonberg,W. Seitz,P. Soliveri,Francis O. Walker,Burgunder J-M.,I. Romero,A Magara,Y Stebler,Hugh Rickards,J. Wright,J. de Souza,Roger A. Barker,Sarah Mason,A. Di Pietro,Andrew D. Goodman,D. O’Keeffe,M Langlois,G. Ferland,Louis Verret,Sylvain Chouinard,S. Paris,C. Lepage,A H Nemeth,C. Merritt,Christopher Cox,T Astbury,Sinéad M. Murphy,Anwar Ahmed,P St Marie,R A Berila,C Kubu,V Segro,Rajeev Kumar,Diane Erickson,J Schneiders,Steven J. Frucht,Paula Wasserman,Carol Moskowitz,Burton L. Scott,P Perry-Trice,S Wyne,D. Parida,V. Redaelli,Witold Sołtan,Piotr Robowski,M Nowak,Michał Schinwelski,A Dziadkiewicz,Thomasin C. Andrews,D Ruddy,A. Dougherty,K. Boelmans,J Schmalfeld,A Muenchau,S. Zittel,William M. Mallonee,Greg Suter,J Tan,Lauren Seeberger,J. Harris,J. Champion,Joanne Wojcieszek,Joann Belden,Kathy Price,M Hughes-Gay,G. Sprehn,Ferdinando Squitieri,T. Martino,F De Gregorio,A De Nicola,F Elifani,Adam Rosenblatt,Nadine Yoritomo,Russell L. Margolis,Paige Nichols,S E Palhagen,A V Hoglund,M Paucar,T W Reza-Soltani,A Beister,T Raab,J Kieni,C. Schrenk,K Banaszkiewicz,J Misztela,M. Wójcik,E Szczygiel,M Golosz,M. Rudzinska,Roos Rac.,van den Bogaard Sja.,R Bos,S J Booij,Christopher Hyson,J. Megens,E Makaji,Mary E. Jenkins,Steven M. Hersch,S Maya,C Dresser,Diana Rosas,Karen Blindauer,C. Schindler,S. Hung,A A McNees,Sarah J. Tabrizi,M Novak,M Say,Anil D. Patel,Peter Panegyres,N. Lewis,S Jukich,C. Faull,L E Hjermind,Ø. Jakobsen,A. Vogel,T R Nielsen,Jørgen E. Nielsen,Sandra K. Kostyk,A. Seward,P Agrawal,J Kraakevik,Penelope Hogarth,A. Wilson,J. Lear,P. H. Kraus,Carsten Saft,T. Steiner,R Hoffmann,C. Stamm,J. Schöllhammer,I. Uhl,B. Kamiński,K. O’Donovan,Oliver Quarrell,L. Nevitt,C. Kipps,A Hare,K Gunner,E. Hayward,M. Nance,J Hamerlinck,Catherine L. Wielinski,Olga Yastrubetskaya,E Chiu,P. Chua,B Mannaa,M. de Tommaso,C Serpino,C Cormio,V Sciruicchio,G. De Michele,L. Di Maio,C V Russo,F. Sacca,E. Salvatore,T. Tucci,M. Wolz,L Klingelhoefer,A Wolz,S. Schmidt,A Storch,E Spruth,S. Thiel,B. Neumann,H. Gelderblom,Josef Priller,Christian Sass,D. Probst,C. Werner,Blair R. Leavitt,Allison Coleman,Lynn A. Raymond,Vicki Wheelock,T. Tempkin,K Baynes,Neal Hermanowicz,Shari Niswonger,M Haske-Palomino,Yvette Bordelon,A Gratiano,A Johnson,Jody Corey-Bloom,Jody Goldstein,Guerry M. Peavy,Michael D. Geschwind,Jonathan Gooblar,C Barton,Hubert H. Fernandez,Ramon L. Rodriguez,M Suelter,M. Daniels,J Romrell,Camille Swartz,Leigh J. Beglinger,Eric A. Epping,E. Waterman,Megan M. Smith,Richard Dubinsky,H Dubinsky,Carolyn Gray,David Craufurd,E Howard,M. Jones,H. Murphy,Karen E. Anderson,C. Nickerson,J De Santo,T. Rigaud,N Zappala,B. Robottom,Carlos Singer,Monica Quesada,K Rodriguez-Spengler,R H Cardenache,Ralf Reilmann,S. Bohlen,Hoelzner E-M.,Amy Colcher,H Maccarone,L Altin,Andrew Siderowf,Timothy Greenamyre,N. Lucarelli,L. Ivanco,Frederick Marshall,Charlyne Hickey,Lisa M. Deuel,Kevin M. Biglan,Sigurd D. Süssmuth,Michael Orth,Sonja Trautmann,Carolin Eschenbach,Ali Samii,Alma Macaraeg,D. Zielonka,A. Ciesielska,J. T. Marcinkowski,J Sempolowicz,H Karaskiewicz,C. ONeill,Ihtsham Haq,G. Witkowski,J. Antczak,R. Rola,P. Richter,M. Rakowicz,K Jachinska,Susan R. Criswell,P Deppen,K. Wharton,N Mahant,Elizabeth McCusker,Jane Griffith,C. Loy,L. Stewart,D. Fisher,D. Holt,Constance Orme,Arthur Watts,Weber J,K. White,Robert A. Hauser,Roger L. Albin,Christopher S. Coffey,William Fischer,Janis Miyasaki,Investigators Horizon.

A randomized, double-blind, placebo-controlled study of latrepirdine in patients with mild to moderate Huntington disease.

2013

BACKGROUND Latrepirdineis an orally administered experimental small molecule that was initially developed as an antihistamine and subsequently was shown to stabilize mitochondrial membranes and function, which might be impaired in Huntington disease. OBJECTIVE To determine the effect of latrepirdineon cognition and global function in patients with mild to moderate Huntington disease. DESIGN Randomized, double-blind, placebo-controlled study. SETTING Sixty-four research centers in Australia, Europe, and North America. PATIENTS Four hundred three patients with mild to moderate Huntington disease and baseline cognitive impairment ( Mini-Mental State Examinationscore, 10-26). INTERVENTION Latrepirdine(20 mg) vs matching placebo administered orally 3 times daily for 26 weeks. MAIN OUTCOME MEASURES The co-primary outcome measures were cognition as measured by the change in Mini-Mental State Examinationscore from baseline to week 26 and global function at week 26 as measured by the Clinician Interview-Based Impression of Change, plus carer interview, which ranges from 1 (marked improvement) to 7 (marked worsening). Secondary efficacy outcome measures included behavior, daily function, motor function, and safety. RESULTS The mean change in Mini-Mental State Examinationscore among participants randomized to latrepirdine(1.5-point improvement) did not differ significantly from that among participants randomized to placebo (1.3-point improvement) (P=.39). Similarly, the distribution of the Clinician Interview-Based Impression of Change, plus carer interview did not differ significantly among those randomized to latrepirdinecompared with placebo (P=.84). No significant treatment effects were detected on the secondary efficacy outcome measures. The incidence of adverse events was similar between those randomized to latrepirdine(68.5%) and placebo (68.0%). CONCLUSION In patients with mild to moderate Huntington disease and cognitive impairment, treatment with latrepirdinefor 6 months was safe and well tolerated but did not improve cognition or global function relative to placebo. TRIAL REGISTRATION clinicaltrials.gov Identifier: NCT00920946.

Keywords:

Correction
Source
Cite
Save

References

Citations