Modeling Disease Progression and Placebo Response in Huntington Disease: Insights From Enroll-HD and GENERATION HD1 Cohorts

Marcelo Boareto; Yumi Yamamoto; Jeffrey D Long; Cristina Sampaio; Peter McColgan; Cheikh Diack; Patricia Sanwald Ducray

doi:10.1212/WNL.0000000000213646

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Modeling Disease Progression and Placebo Response in Huntington Disease: Insights From Enroll-HD and GENERATION HD1 Cohorts

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Modeling Disease Progression and Placebo Response in Huntington Disease: Insights From Enroll-HD and GENERATION HD1 Cohorts

Marcelo Boareto, Yumi Yamamoto, Jeffrey D Long, Cristina Sampaio, Peter McColgan, Cheikh Diack and Patricia Sanwald Ducray

Neurology, Vol.104(10), e213646

05/27/2025

DOI: 10.1212/WNL.0000000000213646

PMCID: PMC12057022

PMID: 40315394

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Abstract

Huntington disease is a rare neurodegenerative disorder with no disease-modifying therapies. This study aimed to quantify longitudinal changes in Unified Huntington's Disease Rating Scale (UHDRS) scores and evaluate their susceptibility to placebo response, enhancing our understanding of disease progression and ability to optimize future trials. We used data from the Enroll-HD natural history study (NCT01574053) and the GENERATION HD1 phase 3 clinical trial (NCT03761849) to model disease progression and placebo response for UHDRS scores, which are commonly used to evaluate disease progression in clinical trials. We included 8,071 Enroll-HD participants (mean baseline age: 51.4 years, 51.5% female) to develop a natural history progression model using baseline characteristics as predictive covariates. This model was then used to predict natural history progression of 260 participants from the GENERATION HD1 placebo arm (mean baseline age: 48.7 years, 43.5% female).The progression measured by Total Functional Capacity (TFC) in the GENERATION HD1 placebo arm aligned with predicted natural history (within 95% CI), indicating no significant placebo response. However, significant improvements (outside the 95% CI of the model) were observed after baseline for Total Motor Score (TMS), Symbol Digit Modalities Test (SDMT) score, and Stroop Word Reading (SWR) score. The improvement in TMS persisted until the end of the dosing period (week 69), converging to natural history predictions at subsequent follow-up visits (weeks 85 and 101), suggesting a placebo effect. By contrast, cognitive scores (SDMT and SWR) showed sustained significant improvement (outside the 95% CI) up to the final follow-up visit at week 101, likely due to practice effects from the more frequent testing schedule in GENERATION HD1 compared with the annual assessments in Enroll-HD. Consequently, the composite UHDRS (cUHDRS) score, a linear combination of TFC, TMS, SDMT, and SWR, is influenced by both placebo and practice effects. Our results suggest that clinical scores in Huntington disease trials are susceptible to long-term placebo responses. These effects should be considered in future trial designs, especially when comparing trial data with natural history studies. Although based on the largest Huntington's trial, our results rely on limited placebo data and may not generalize to other trials with different populations, treatments, and designs.

Adult

Cohort Studies

Disease Progression

Female

Humans

Huntington Disease - diagnosis

Huntington Disease - drug therapy

Huntington Disease - physiopathology

Huntington Disease - psychology

Male

Middle Aged

Placebo Effect

Details

Title: Subtitle: Modeling Disease Progression and Placebo Response in Huntington Disease: Insights From Enroll-HD and GENERATION HD1 Cohorts
Creators: Marcelo Boareto - Roche Pharma Research and Early Development (pRED), F. Hoffmann-La Roche Ltd., Basel, Switzerland
Yumi Yamamoto - Roche Pharma Research and Early Development (pRED), F. Hoffmann-La Roche Ltd., Basel, Switzerland
Jeffrey D Long - Department of Biostatistics, University of Iowa, Iowa City
Cristina Sampaio
Peter McColgan - Roche (United Kingdom)
Cheikh Diack - Roche Pharma Research and Early Development (pRED), F. Hoffmann-La Roche Ltd., Basel, Switzerland
Patricia Sanwald Ducray - Roche Pharma Research and Early Development (pRED), F. Hoffmann-La Roche Ltd., Basel, Switzerland
Resource Type: Journal article
Publication Details: Neurology, Vol.104(10), e213646
DOI: 10.1212/WNL.0000000000213646
PMID: 40315394
PMCID: PMC12057022
NLM abbreviation: Neurology
ISSN: 1526-632X
eISSN: 1526-632X
Publisher: Lippincott Williams & Wilkins; PHILADELPHIA
Grant note: CHDI Foundation, Inc.CHDI Foundation
Natural history data used in this work were generously provided by the participants in the Enroll-HD study and made available by CHDI Foundation, Inc. Enroll-HD is a clinical research platform and longitudinal observational study for families with Huntington disease intended to accelerate progress toward therapeutics; it is sponsored by CHDI Foundation, a nonprofit biomedical research organization exclusively dedicated to collaboratively developing therapeutics for HD. Enroll-HD would not be possible without the vital contribution of the research participants and their families. The authors thank all CHDI/Enroll-HD participants and all the participants in GENERATION HD1, their families, the site staff, and the trial team, for their time and commitment to the trial, and the following colleagues and HD experts for their critical feedback on method development and discussions: Francesco Brizzi, Tony Kam-Thong, Antoine Soubret, Ben Ribba, and David Hawellek.
Language: English
Date published: 05/27/2025
Academic Unit: Psychiatry; Biostatistics
Record Identifier: 9984815910502771

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