Clinical manifestations of homozygote allele carriers in Huntington disease

Cubo, Esther; Martinez-Horta, Saul-Indra; Sampedro, Frederic; Descalls, Asunción Martínez; Calvo, Sara; Gil‐Polo, Cecilia; Muñoz, Ignacio Cano; Llano, Katia; Mariscal, Natividad; Dı́az, Dolores; Gutierrez, Aranzazu; Aguado, Laura; Ramos-Arroyo, María A.

doi:10.1212/wnl.0000000000007147

Cited by 28 publications

(13 citation statements)

References 29 publications

(41 reference statements)

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“…Although certainly attractive, this hypothesis fails to explain two groups of data. First, it does not explain why the age of onset of dominant HD is well-predicted by the length of the longer repeat expansion allele in homozygous patients (243,244) or why the age of onset of recessive FRDA is determined solely by the shorter GAA expansion allele JBC REVIEWS: Repeat-mediated genome instability (245)(246)(247). Second, it fails to explain why the age of onset of HD is better predicted by the length of noninterrupted CAG repeats in DNA rather than by the length of the polyQ tract in the protein (128 -130).…”

Section: Length Instability In Somatic Tissuesmentioning

confidence: 99%

On the wrong DNA track: Molecular mechanisms of repeat-mediated genome instability

Khristich

Mirkin

2020

Journal of Biological Chemistry

197

229

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Expansions of simple tandem repeats are responsible for almost 50 human diseases, the majority of which are severe, degenerative, and not currently treatable or preventable. In this review, we first describe the molecular mechanisms of repeat-induced toxicity, which is the connecting link between repeat expansions and pathology. We then survey alternative DNA structures that are formed by expandable repeats and review the evidence that formation of these structures is at the core of repeat instability. Next, we describe the consequences of the presence of long structure-forming repeats at the molecular level: somatic and intergenerational instability, fragility, and repeat-induced mutagenesis. We discuss the reasons for gender bias in intergenerational repeat instability and the tissue specificity of somatic repeat instability. We also review the known pathways in which DNA replication, transcription, DNA repair, and chromatin state interact and thereby promote repeat instability. We then discuss possible reasons for the persistence of disease-causing DNA repeats in the genome. We describe evidence suggesting that these repeats are a payoff for the advantages of having abundant simple-sequence repeats for eukaryotic genome function and evolvability. Finally, we discuss two unresolved fundamental questions: (i) why does repeat behavior differ between model systems and human pedigrees, and (ii) can we use current knowledge on repeat instability mechanisms to cure repeat expansion diseases?

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Section: Length Instability In Somatic Tissuesmentioning

confidence: 99%

On the wrong DNA track: Molecular mechanisms of repeat-mediated genome instability

Khristich

Mirkin

2020

Journal of Biological Chemistry

197

229

View full text Add to dashboard Cite

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“…Indeed, HTT alleles with 37 repeats are considered pathogenic with reduced penetrance (37 < CAG < 40). Nevertheless, biallelic HD patients do not display significant differences in disease onset or progression compared to those harboring a single mutated allele, 16 supporting the “complete dominance” of HD.…”

Section: Discussionmentioning

confidence: 85%

Analysis of HTT CAG repeat expansion in Italian patients with amyotrophic lateral sclerosis

Manini

Gagliardi

Meneri

et al. 2022

Ann Clin Transl Neurol

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HTT full-penetrance pathogenic repeat expansions, the genetic cause of Huntington's disease (HD), have been recently reported in a minority of frontotemporal dementia/amyotrophic lateral sclerosis (ALS) patients (0.13%). We analyzed HTT CAG repeats in an Italian cohort of ALS patients (n = 467) by repeat-primed polymerase chain reaction. One patient harbored two expanded alleles in the HTT gene (42 and 37 CAG repeats). The absence of HD typical symptoms and the clinical picture consistent with ALS, corroborated by the diagnostic assessment, apparently excluded a misdiagnosis of HD.

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“…Huntington’s disease is caused predominantly by an expansion of trinucleotide CAG repeats in the huntingtin gene ( HTT ; OMIM #613004) [92]. Huntington’s disease is a true autosomal dominant condition because the clinical phenotype of a homozygote is indistinguishable from that of a heterozygote [93]. Nonetheless, it is the number of CAG repeats that determines the age of onset of disease, as well as its progression and severity.…”

Section: Resultsmentioning

confidence: 99%

Validation of the ACMG/AMP guidelines-based seven-category variant classification system

Chen

Masson

Zou

et al. 2023

Preprint

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Background:One shortcoming of employing the American College of Medical Genetics and Genomics/Association for Molecular Pathology (ACMG/AMP)-recommended five-category variant classification scheme (″pathogenic″, ″likely pathogenic″, ″uncertain significance″, ″likely benign″ and ″benign″) in medical genetics lies in the schemeprime or minutes inherent inability to deal properly with variants that fall midway between ″pathogenic″ and ″benign″. Employing chronic pancreatitis as a disease model, and focusing on the four most studied chronic pancreatitis-related genes, we recently expanded the five-category ACMG/AMP scheme into a seven-category variant classification system. With the addition of two new classificatory categories, ″predisposing″ and ″likely predisposing″, our seven-category system promises to provide improved classification for the entire spectrum of variants in any disease-causing gene. The applicability and practical utility of our seven-category variant classification system however remains to be demonstrated in other disease/gene contexts, and this has been the aim of the current analysis.Results:We have sought to demonstrate the potential universality of pathological variants that could be ascribed the new variant terminology (′predisposing′) by trialing it across three Mendelian disease contexts (i.e., autosomal dominant, autosomal recessive and X-linked). To this end, we firstly employed illustrative genes/variants characteristic of these three contexts. On the basis of our own knowledge and expertise, we identified a series of variants that fitted well with our ″predisposing″ category, including ″hypomorphic″ variants in thePKD1gene and ″variants of varying clinical consequence″ in theCFTRgene. These examples, followed by reasonable extrapolations, enabled us to infer the widespread occurrence of ″predisposing″ variants in disease-causing genes. Such ″predisposing″ variants are likely to contribute significantly to the complexity of human genetic disease and may account not only for a considerable proportion of the unexplained cases of monogenic and oligogenic disease but also for much of the ″missing heritability″ characteristic of complex disease.Conclusion:Employing an evidence-based approach together with reasonable extrapolations, we demonstrate both the applicability and utility of our seven-category variant classification system for disease-causing genes. The recognition of the new ″predisposing″ category not only has immediate implications for variant detection and interpretation but should also have important consequences for reproductive genetic counseling.

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Clinical manifestations of homozygote allele carriers in Huntington disease

Cited by 28 publications

References 29 publications

On the wrong DNA track: Molecular mechanisms of repeat-mediated genome instability

On the wrong DNA track: Molecular mechanisms of repeat-mediated genome instability

Analysis of HTT CAG repeat expansion in Italian patients with amyotrophic lateral sclerosis

Validation of the ACMG/AMP guidelines-based seven-category variant classification system

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