Huntington's Disease with Small CAG Repeat Expansions

Background Carriers of small cytosine‐adenine‐guanine (CAG) repeats below 39 in the HTT gene are traditionally associated with milder Huntington's disease, but their clinical profile has not been extensively studied. Objective To study the phenotype of CAG36‐38 repeat carriers. Methods We inclu...

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Published in:Movement disorders 2023-07, Vol.38 (7), p.1294-1306
Main Authors: Heinzmann, Anna, Sayah, Sabrina, Lejeune, François‐Xavier, Hahn, Valérie, Teichmann, Marc, Monin, Marie‐Lorraine, Marchionni, Enrica, Gérard, Fleur, Charles, Perrine, Pariente, Jérémie, Durr, Alexandra
Format: Article
Language:English
Subjects:
Chorea
Chorea - complications
Cognitive ability
cognitive decline
Cytosine
Diagnosis
Genetic counseling
Heterozygote
Human health and pathology
Humans
Huntington Disease
Huntington Disease - diagnosis
Huntington's disease
Huntingtons disease
Life Sciences
Movement disorders
Phenotype
Phenotypes
Polyglutamine
reduced penetrance
small expansions
Trinucleotide repeat diseases
Trinucleotide repeats
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Summary:Background Carriers of small cytosine‐adenine‐guanine (CAG) repeats below 39 in the HTT gene are traditionally associated with milder Huntington's disease, but their clinical profile has not been extensively studied. Objective To study the phenotype of CAG36‐38 repeat carriers. Methods We included 35 patients and premanifest carriers of CAG36‐38 repeats. We compared clinical and neuropsychological profiles of 11 CAG36‐38 patients with 11 matched CAG40‐42 patients. In addition, we analyzed 243 CAG36‐38 individuals from the ENROLL study to complete the phenotype description. Results Global cognitive efficiency and performance in different cognitive subdomains were similar in small CAG36‐38 and typically CAG40‐42 expanded individuals. Chorea as the first symptom was significantly less frequent for CAG36‐38 patients (P = 0.04) despite similar total motor scores at first visit. Total motor score at last visit was significantly lower in CAG36‐38 carriers (P = 0.003). The similar cognitive and different motor profile of CAG36‐38 (n = 243) and CAG40‐42 (n = 4675) carriers was confirmed in the ENROLL database. Additionally, clinicians were significantly less confident in diagnosing Huntington's disease (P = 2.4e−8) and diagnosis happened significantly later in CAG36‐38 (P = 2.2e−6) despite a similar age at symptom onset (P = 0.29). Conclusions We showed that small CAG36‐38 expansion carriers had a similar cognitive profile to those with the more common CAG40‐42 expansions. These individuals may evade molecular diagnosis because of the absence of chorea rather than because of a low penetrance of symptoms. This finding should encourage neurologists to consider Huntington's disease in cognitively impaired elderly patients without typical chorea and anticipate consequences for genetic counseling in their offspring. © 2023 The Authors. Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.
ISSN:0885-3185
1531-8257
DOI:10.1002/mds.29427