Molecular diagnosis of Huntington disease in Portugal: implications for genetic counselling and clinical practice

Costa, Maria do Carmo; Magalhães, Paula; Ferreirinha, Fátima; Guimarães, Laura; Januário, Cristina; Gaspar, Isabel; Loureiro, José Leal; Vale, José; Garrett, Carolina; Regateiro, Fernando; Magalhães, Marina; Sousa, Alda; Maciel, Patrı́cia; Sequeiros, Jorge

doi:10.1038/sj.ejhg.5201055

Cited by 22 publications

(28 citation statements)

References 25 publications

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“…The presence of these two mutated alleles in a randomly selected sample of 1,000 individuals from our population could correspond to a higher prevalence of HD in the Portuguese population than described elsewhere. In a previous report, we had predicted it to be at least 2-5:10,0000 (Costa et al 2003), i.e. similar to that of other European countries.…”

Section: Discussionsupporting

confidence: 77%

“…In addition, haplotype analyses in HD families of different ethnic populations has suggested that multiple mutation events underlie this disorder, and that a specific group of normal unstable alleles within a particular haplotype may be more prone to expansion leading to fully penetrant HD alleles, thus constituting a pool for the generation of new HD genes (Goldberg et al 1993;Squitieri et al 1994;Almqvist et al 1995). Previously, from our routine genetic testing in Portugal, we observed that normal unstable alleles (class 2) had a relatively high frequency, accounting for 3.7% of the ''normal'' chromosomes (Costa et al 2003).…”

Section: Introductionmentioning

confidence: 90%

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The CAG repeat at the Huntington disease gene in the Portuguese population: insights into its dynamics and to the origin of the mutation

Costa

Magalhães²,

Guimarães

et al. 2005

J Hum Genet

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Huntington disease (HD) is caused by an expansion of a CAG repeat. This repeat is a dynamic mutation that tends to undergo intergenerational instability. We report the analysis of the CAG repeat in a large population sample (2,000 chromosomes) covering all regions of Portugal, and a haplotype study of (CAG) n and (CCG) n repeats in 140 HD Portuguese families. Intermediate class 2 alleles represented 3.0% of the population; and two expanded alleles (36 and 40 repeats, 0.11%) were found. There was no evidence for geographical clustering of the intermediate or expanded alleles. The Portuguese families showed three different HD founder haplotypes associated with 7-, 9-or 10-CCG repeats, suggesting the possibility of different origins for the HD mutation among this population. The haplotype carrying the 7-CCG repeat was the most frequent, both in normal and in expanded alleles. In general, we propose that three mechanisms, occurring at different times, may lead to the evolution from normal CAGs to full expansion: first, a mutation bias towards larger alleles; then, a stepwise process that could explain the CAG distributions observed in the more recent haplotypes; and, finally, a pool of intermediate (class 2) alleles more prone to give rise to expanded HD alleles.

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Section: Discussionsupporting

confidence: 77%

Section: Introductionmentioning

confidence: 90%

The CAG repeat at the Huntington disease gene in the Portuguese population: insights into its dynamics and to the origin of the mutation

Costa

Magalhães²,

Guimarães

et al. 2005

J Hum Genet

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“…As we have previously reported (Costa et al 2003), among our series of cases for HD diagnosis, we found a high number of HD mutation-negative patients who had both a family history and typical HD clinical features. Here, we describe a series of 107 HDL patients of Portuguese origin, who do not present (CAG) n expansions in the HD gene.…”

Section: Introductionsupporting

confidence: 62%

Exclusion of mutations in the PRNP, JPH3, TBP, ATN1, CREBBP, POU3F2 and FTL genes as a cause of disease in Portuguese patients with a Huntington-like phenotype

et al. 2006

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Huntington disease (HD) is an autosomal dominant neurodegenerative disorder characterised by chorea, cognitive impairment, dementia and personality changes, caused by the expansion of a CAG repeat in the HD gene. Often, patients with a similar clinical presentation do not carry expansions of the CAG repeat in this gene [Huntington disease-like (HDL) patients]. We report the genetic analysis of 107 Portuguese patients with an HDL phenotype. The HDL genes PRNP and JPH3, encoding the prion protein and junctophilin-3, respectively, were screened for repeat expansions in these patients. Given the partial clinical overlap of SCA17, DRPLA and neuroferritinopathy with HD, their causative genes (TBP, ATN1, and FTL, respectively) were also analysed. Finally, repeat expansions in two candidate genes, CREBBP and POU3F2, which encode the nuclear transcriptional coactivator CREB-binding protein and the CNS-specific transcription factor NOct-3, respectively, were also studied. Expansions of the repetitive tracts of the PRNP, JPH3, TBP, ATN1, CREBBP and POU3F2 genes were excluded in all patients, as were sequence alterations in the FTL gene. Since none of the genes already included in the differential diagnosis of HD was responsible for the disease in our sample, the genetic heterogeneity of the HDL phenotype is still open for investigation.

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“…HD was diagnosed in 93% of 618 French and Moroccan (13), 82.8% of 169 Portuguese (14), 57% of 66 Brazilian (15) and 50% of 11 South African black (16) patients with a HDlike phenotype. A review of the literature might suggest a gradient of frequency, where HTT expansions are much more prevalent among North-Europeans, than in other populations.…”

Section: Discussionmentioning

confidence: 99%

Huntington disease and Huntington disease‐like in a case series from Brazil

et al. 2013

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The aim of this study was to identify the relative frequency of Huntington's disease (HD) and HD-like (HDL) disorders HDL1, HDL2, spinocerebellar ataxia type 2 (SCA2), SCA17, dentatorubral-pallidoluysian degeneration (DRPLA), benign hereditary chorea, neuroferritinopathy and chorea-acanthocytosis (CHAC), in a series of Brazilian families. Patients were recruited in seven centers if they or their relatives presented at least chorea, besides other findings. Molecular studies of HTT, ATXN2, TBP, ATN1, JPH3, FTL, NKX2-1/TITF1 and VPS13A genes were performed. A total of 104 families were ascertained from 2001 to 2012: 71 families from South, 25 from Southeast and 8 from Northeast Brazil. There were 93 HD, 4 HDL2 and 1 SCA2 families. Eleven of 104 index cases did not have a family history: 10 with HD. Clinical characteristics were similar between HD and non-HD cases. In HD, the median expanded (CAG)n (range) was 44 (40-81) units; R(2) between expanded HTT and age-at-onset (AO) was 0.55 (p=0.0001, Pearson). HDL2 was found in Rio de Janeiro (2 of 9 families) and Rio Grande do Sul states (2 of 68 families). We detected HD in 89.4%, HDL2 in 3.8% and SCA2 in 1% of 104 Brazilian families. There were no cases of HDL1, SCA17, DRPLA, neuroferritinopathy, benign hereditary chorea or CHAC. Only six families (5.8%) remained without diagnosis.

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Molecular diagnosis of Huntington disease in Portugal: implications for genetic counselling and clinical practice

Cited by 22 publications

References 25 publications

The CAG repeat at the Huntington disease gene in the Portuguese population: insights into its dynamics and to the origin of the mutation

The CAG repeat at the Huntington disease gene in the Portuguese population: insights into its dynamics and to the origin of the mutation

Exclusion of mutations in the PRNP, JPH3, TBP, ATN1, CREBBP, POU3F2 and FTL genes as a cause of disease in Portuguese patients with a Huntington-like phenotype

Huntington disease and Huntington disease‐like in a case series from Brazil

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