Venezuelan kindreds reveal that genetic and environmental factors modulate Huntington's disease age of onset

Wexler, Nancy S.; Lorimer, Judith; Porter, Julie; Gomez, Fidela; Moskowitz, Carol; Shackell, Edith; Marder, Karen; Penchaszadeh, Graciela K.; Roberts, Simone A.; Gayán, Javier; Brocklebank, Denise; Cherny, Stacey S.; Cardon, Lon R.; Gray, Jacqueline S.; Dlouhy, Stephen R.; Wiktorski, Sandra; Hodes, M. E.; Conneally, P. Michael; Penney, JB; Gusella, James F.; Ho, Jang Seung; Irizarry, Michael C.; Rosas, Diana; Hersch, Steven M.; Hollingsworth, Zane R.; MacDonald, Marcy E.; Young, Anne B.; Andresen, J. Michael; Housman, David E.; Young, Margot Mieja De; Bonilla, Ernesto; Stillings, Theresa; Negrette, Américo; Snodgrass, S. Robert; Martinez-Jaurrieta, Maria Dolores; Ramos-Arroyo, María A.; Bickham, Jacqueline; Ramos, Juan Sanchez; Marshall, Frederick J.; Shoulson, Ira; Rey, Gustavo; Feigin, Andrew; Arnheim, Norman; Acevedo-Cruz, Amarilis; Acosta, Leticia; Alvir, José; Fischbeck, Kenneth H.; Thompson, Leslie M.; Young, Angela M.; Dure, Leon S.; O’Brien, Christopher J.; Paulsen, Jane S.; Brickman, Adam M.; Krch, Denise; Peery, Shelley; Hogarth, Penelope; Higgins, Donald S.; Landwehrmeyer, G. Bernhard

doi:10.1073/pnas.0308679101

Cited by 627 publications

(223 citation statements)

References 25 publications

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“…The number of CAG repeats in normal chromosomes is significantly higher in populations presenting high prevalence of HD Squitieri et al, 1994). Higher averages of CAG numbers in normal chromosomes were found in Mexico, Cuba, Brazil, Europe, North America, and Oceania (Raskin et al, 2000;Wexler et al, 2004;McNicoll et al, 2008;Alonso et al, 2009;Semaka et al, 2013b;Vázquez-Mojena et al, 2013).…”

Section: Discussionmentioning

confidence: 81%

REVIEW-ARTICLE Intermediate alleles of Huntington’s disease HTT gene in different populations worldwide: a systematic review

2017

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ABSTRACT. Huntington's disease (HD) is an autosomal dominant progressive neurodegenerative disorder caused by a dynamic mutation due to the expansion of CAG repeats in the HTT gene (4p16.3). The considered normal alleles have less than 27 CAG repeats. Intermediate alleles (IAs) show 27 to 35 CAG repeats and expanded alleles have more than 35 repeats. The IAs apparently have shown a normal phenotype. However, there are some reported associations between individuals that bear an IA and clinical HD signs, such as behavioral disturbs. The association of IAs with the presence of clinical signs gives clinical relevance to these patients. We emphasized the importance of determining the frequency of IA alleles in the general population as well as in HD families. Therefore, the aim of this study was to conduct a systematic review, in order to investigate the frequency of IAs in the overall chromosomes of different ethnic groups and of families with HD history worldwide as well as the frequency of individuals who bear the intermediate alleles. We searched indexed articles from the following electronic databases: U.S. National Library of Medicine and the National Institutes of Health (PubMed), Pubmed Central (PMC) and Virtual Health Library (VHL). Therefore, 488 articles were obtained and, of these, 33 had been published in more than one database. We accepted the article of only one database and ended up with 455 articles for this review. The frequency of IAs within the chromosomes of the general population ranged from 0.45 to 8.7% and of individuals with family history of HD ranged from 0.05 to 5.1%. The higher frequency of IAs in the general population (8.7%) was found in one Brazilian cohort.

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Section: Discussionmentioning

confidence: 81%

REVIEW-ARTICLE Intermediate alleles of Huntington’s disease HTT gene in different populations worldwide: a systematic review

2017

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“…Classically, age at onset was established on the basis of 'score equal to 4', according to the DCL of the United Huntington' s Disease Rating Scale (UHDRS) in a mutation carrier subject 19 . Nevertheless, several reports on pre-manifest subjects remarked the occurrence of non-motor behavioral and cognitive manifestations anticipating the typical motor signs and symptoms by even many years 19,20,21,22,23 , thus making the definition of age at onset in JHD still controversial 5,6,19,20,21,22,23 . Recently, Reilmann et al, suggested to take in account the whole individual medical history, i.e.…”

Section: Discussionmentioning

confidence: 99%

“…Nevertheless, we believe that this series may contribute to the expansion of knowledge of the JHD variant, which is already rare and, particularly so, due to the limited number of reports focusing on this topic from South America, with the exception of the Venezuelan community 23 .…”

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confidence: 99%

Juvenile Huntington disease in Argentina

Gatto

Parisi

Etcheverry³

et al. 2015

Arq. Neuro-Psiquiatr.

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We analyzed demographic, clinical and genetic characteristics of juvenile Huntington disease (JHD) and it frequency in an Argentinean cohort. Age at onset was defined as the age at which behavioral, cognitive, psychiatric or motor abnormalities suggestive of JHD were first reported. Clinical and genetic data were similar to other international series, however, in this context we identified the highest JHD frequency reported so far (19.72%; 14/71). Age at onset of JHD is challenging and still under discussion. Our findings reinforce the hypothesis that clinical manifestations, other than the typical movement disorder, may anticipate age at onset of even many years. Analyses of JHD cohorts are required to explore it frequency in populations with different backgrounds to avoid an underestimation of this rare phenotype. Moreover, data from selected populations may open new pathways in therapeutic approaches and may explain new potential correlations between HD presentations and environmental or biological factors.

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“…The expansion length is variable and explains much of the heterogeneity in the age at which mutation‐carriers receive a clinical diagnosis of manifest disease (Duyao et al, 1993). A large portion of variability in age at onset, however, remains unexplained by the gene‐mutation and is likely the result of other factors, both genetic and environmental (Wexler et al, 2004). Identifying these factors and their associated biological processes could provide additional targets for therapeutic interventions that may modify disease progression.…”

Section: Introductionmentioning

confidence: 99%

Natural biological variation of white matter microstructure is accentuated in Huntington's disease

Gregory

Crawford

Seunarine

et al. 2018

Human Brain Mapping

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Huntington's disease (HD) is a monogenic neurodegenerative disorder caused by a CAG‐repeat expansion in the Huntingtin gene. Presence of this expansion signifies certainty of disease onset, but only partly explains age at which onset occurs. Genome‐wide association studies have shown that naturally occurring genetic variability influences HD pathogenesis and disease onset. Investigating the influence of biological traits in the normal population, such as variability in white matter properties, on HD pathogenesis could provide a complementary approach to understanding disease modification. We have previously shown that while white matter diffusivity patterns in the left sensorimotor network were similar in controls and HD gene‐carriers, they were more extreme in the HD group. We hypothesized that the influence of natural variation in diffusivity on effects of HD pathogenesis on white matter is not limited to the sensorimotor network but extends to cognitive, limbic, and visual networks. Using tractography, we investigated 32 bilateral pathways within HD‐related networks, including motor, cognitive, and limbic, and examined diffusivity metrics using principal components analysis. We identified three independent patterns of diffusivity common to controls and HD gene‐carriers that predicted HD status. The first pattern involved almost all tracts, the second was limited to sensorimotor tracts, and the third encompassed cognitive network tracts. Each diffusivity pattern was associated with network specific performance. The consistency in diffusivity patterns across both groups coupled with their association with disease status and task performance indicates that naturally‐occurring patterns of diffusivity can become accentuated in the presence of the HD gene mutation to influence clinical brain function.

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Venezuelan kindreds reveal that genetic and environmental factors modulate Huntington's disease age of onset

Cited by 627 publications

References 25 publications

REVIEW-ARTICLE Intermediate alleles of Huntington’s disease HTT gene in different populations worldwide: a systematic review

REVIEW-ARTICLE Intermediate alleles of Huntington’s disease HTT gene in different populations worldwide: a systematic review

Juvenile Huntington disease in Argentina

Natural biological variation of white matter microstructure is accentuated in Huntington's disease

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