PT - JOURNAL ARTICLE AU - McAllister, Branduff AU - Gusella, James F. AU - Landwehrmeyer, G. Bernhard AU - Lee, Jong-Min AU - MacDonald, Marcy E. AU - Orth, Michael AU - Rosser, Anne E. AU - Williams, Nigel M. AU - Holmans, Peter AU - Jones, Lesley AU - Massey, Thomas H. AU - , TI - Timing and Impact of Psychiatric, Cognitive, and Motor Abnormalities in Huntington Disease AID - 10.1212/WNL.0000000000011893 DP - 2021 May 11 TA - Neurology PG - e2395--e2406 VI - 96 IP - 19 4099 - http://n.neurology.org/content/96/19/e2395.short 4100 - http://n.neurology.org/content/96/19/e2395.full SO - Neurology2021 May 11; 96 AB - Objective To assess the prevalence, timing, and functional impact of psychiatric, cognitive, and motor abnormalities in Huntington disease (HD) gene carriers, we analyzed retrospective clinical data from individuals with manifest HD.Methods Clinical features of patients with HD were analyzed for 6,316 individuals in an observational study of the European Huntington's Disease Network (REGISTRY) from 161 sites across 17 countries. Data came from clinical history and the patient-completed Clinical Characteristics Questionnaire that assessed 8 symptoms: motor, cognitive, apathy, depression, perseverative/obsessive behavior, irritability, violent/aggressive behavior, and psychosis. Multiple logistic regression was used to analyze relationships between symptoms and functional outcomes.Results The initial manifestation of HD is increasingly likely to be motor and less likely to be psychiatric as age at presentation increases and is independent of pathogenic CAG repeat length. The Clinical Characteristics Questionnaire captures data on nonmotor symptom prevalence that correlate specifically with validated clinical measures. Psychiatric and cognitive symptoms are common in HD gene carriers, with earlier onsets associated with longer CAG repeats. Of patients with HD, 42.4% reported at least 1 psychiatric or cognitive symptom before motor symptoms, with depression most common. Each nonmotor symptom was associated with significantly reduced total functional capacity scores.Conclusions Psychiatric and cognitive symptoms are common and functionally debilitating in HD gene carriers. They require recognition and targeting with clinical outcome measures and treatments. However, because it is impossible to distinguish confidently between nonmotor symptoms arising from HD and primary psychiatric disorders, particularly in younger premanifest patients, nonmotor symptoms should not be used to make a clinical diagnosis of HD.Trial Registration Information ClinicalTrials.gov Identifier: NCT01590589CI=confidence interval; EHDN=European Huntington's Disease Network; HADS=Hospital Anxiety/Depression Scale; HD=Huntington disease; HDCCQ=HD Clinical Characteristics Questionnaire; ICD-10=International Classification of Disease, 10th revision; OR=odds ratio; PBA-s=short form of the Problem Behaviours Assessment; PREDICT-HD=Neurobiological Predictors of Huntington's Disease; REGISTRY=An Observational Study of the European Huntington's Disease Network; SDMT=Symbol-Digit Modalities Test; SIS=Snaith Irritability Scale; TFC=total functional capacity; TMS=total motor score; UHDRS=Unified Huntington's Disease Rating Scale