TY - JOUR
T1 - Challenges assessing clinical endpoints in early Huntington disease
AU - The PREDICT-HD Investigators of the Huntington Study Group
AU - Paulsen, Jane S.
AU - Wang, Chiachi
AU - Duff, Kevin
AU - Barker, Roger
AU - Nance, Martha
AU - Beglinger, Leigh
AU - Moser, David
AU - Williams, Janet K.
AU - Simpson, Sheila
AU - Langbehn, Douglas
AU - van Kammen, Daniel P.
AU - Paulson, Henry
AU - Bastic, Kimberly
AU - Conybeare, Rachel
AU - Humphreys, Clare
AU - Elbert, Mackenzie
AU - Nopoulos, Peg
AU - Rodnitzky, Robert
AU - Uc, Ergun
AU - Beglinger, Leigh
AU - Duff, Kevin
AU - Magnotta, Vincent A.
AU - Cross, Stephen
AU - Doucette, Nicholas
AU - French, Sarah
AU - Hale, Nancy
AU - Juhl, Andrew
AU - Kuburas, Harisa
AU - Mikos, Ania
AU - Reese, Becky
AU - Turner, Beth
AU - Van Der Heiden, Sara
AU - Ames, David
AU - Chiu, Edmond
AU - Chua, Phyllis
AU - Yastrubetskaya, Olga
AU - Dingjan, Phillip
AU - Draper, Kristy
AU - Georgiou-Karistianis, Nellie
AU - Goh, Anita
AU - Komiti, Angela
AU - Lemmon, Christel
AU - Raymond, Lynn
AU - Decolongon, Joji
AU - Rosenblatt, Adam
AU - Ross, Christopher
AU - Agarwal, Abhijit
AU - Gourley, Lisa
AU - Perlmutter, Joel
AU - Mazzoni, Pietro
PY - 2010/11/1
Y1 - 2010/11/1
N2 - The basic aim of this study was to evaluate the current accepted standard clinical endpoint for the earliest-studied HD participants likely to be recruited into clinical trials. As the advent of genetic testing for HD, it is possible to identify gene carriers before the diagnosis of disease, which opens up the possibility of clinical trials of disease-modifying treatments in clinically asymptomatic persons. Current accepted standard clinical endpoints were examined as part of a multinational, 32-site, longitudinal, observational study of 786 research participants currently in the HD prodrome (gene-positive but not clinically diagnosed). Clinical signs and symptoms were used to prospectively predict functional loss as assessed by current accepted standard endpoints over 8 years of follow-up. Functional capacity measures were not sensitive for HD in the prodrome; over 88% scored at ceiling. Prospective evaluation revealed that the first functional loss was in their accustomed work. In a survival analysis, motor, cognitive, and psychiatric measures were all predictors of job change. To our knowledge, this is the first prospective study ever conducted on the emergence of functional loss secondary to brain disease. We conclude that future clinical trials designed for very early disease will require the development of new and more sensitive measures of real-life function.
AB - The basic aim of this study was to evaluate the current accepted standard clinical endpoint for the earliest-studied HD participants likely to be recruited into clinical trials. As the advent of genetic testing for HD, it is possible to identify gene carriers before the diagnosis of disease, which opens up the possibility of clinical trials of disease-modifying treatments in clinically asymptomatic persons. Current accepted standard clinical endpoints were examined as part of a multinational, 32-site, longitudinal, observational study of 786 research participants currently in the HD prodrome (gene-positive but not clinically diagnosed). Clinical signs and symptoms were used to prospectively predict functional loss as assessed by current accepted standard endpoints over 8 years of follow-up. Functional capacity measures were not sensitive for HD in the prodrome; over 88% scored at ceiling. Prospective evaluation revealed that the first functional loss was in their accustomed work. In a survival analysis, motor, cognitive, and psychiatric measures were all predictors of job change. To our knowledge, this is the first prospective study ever conducted on the emergence of functional loss secondary to brain disease. We conclude that future clinical trials designed for very early disease will require the development of new and more sensitive measures of real-life function.
KW - Clinical endpoints
KW - Functional capacity
KW - Huntington disease
KW - Prodromal HD
KW - UHDRS
UR - http://www.scopus.com/inward/record.url?scp=78349250529&partnerID=8YFLogxK
U2 - 10.1002/mds.23337
DO - 10.1002/mds.23337
M3 - Article
C2 - 20623772
AN - SCOPUS:78349250529
SN - 0885-3185
VL - 25
SP - 2595
EP - 2603
JO - Movement Disorders
JF - Movement Disorders
IS - 15
ER -