Your search keyword '"intermediate alleles"' showing total 8 results

1. Incidence of Huntington disease in a northeastern Spanish region: a 13-year retrospective study at tertiary care centre

Author

Juan Pelegrín Sánchez Marín, Silvia Izquierdo Álvarez, Paula Sienes Bailo, and Raquel Lahoz

Subjects

Adult, Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Population, Gene Expression, Disease, 030105 genetics & heredity, Tertiary Care Centers, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Epidemiology, Genetics, medicine, Humans, Allele, education, Predictive testing, Alleles, Genetics (clinical), Aged, Retrospective Studies, Huntingtin Protein, Molecular Epidemiology, education.field_of_study, business.industry, Incidence, Incomplete penetrance alleles, Incidence (epidemiology), Retrospective cohort study, Middle Aged, Huntington disease, HTT gene, Penetrance, Spain, Female, Intermediate alleles, Trinucleotide Repeat Expansion, business, 030217 neurology & neurosurgery, Research Article

Abstract

Background Despite the progress in the knowledge of Huntington disease (HD) in recent years, the epidemiology continues uncertain, so the study of incidence becomes relevant. This is important since various factors (type of population, diagnostic criteria, disease-modifying factors, etc.) make these data highly variable. Therefore, the genetic diagnosis of these patients is important, since it unequivocally allows the detection of new cases. Methods Descriptive retrospective study with 179 individuals. Incidence of HD was calculated from the ratio of number of symptomatic cases newly diagnosed per 100,000 inhabitants per year during the period 2007–2019 in Aragon (Spain). Results 50 (27.9%) incident cases of HD (CAG repeat length ≥ 36) were identified from a total of 179 persons studied. The remaining 129/179 (72.1%) were HD negative (CAG repeat length Conclusions Our incidence lied within the range reported for other Caucasian populations. Implementation of new techniques has allowed to determine the exact number of CAG repeats, which is especially important in patients with triplet expansions in an HD intermediate and/or incomplete penetrance allele, both in diagnostic, predictive and prenatal tests.

Published

2020

2. Evidence-based genetic counselling implications for Huntington disease intermediate allele predictive test results.

Author

Semaka, A. and Hayden, M.R.

Subjects

*GENETIC counseling, *HUNTINGTON disease, *GERM cells, *GENETIC mutation, *GENOTYPE-environment interaction

Abstract

Intermediate alleles ( IAs) for Huntington disease ( HD) contain 27-35 CAG repeats, a range that falls just below the disease threshold of 36 repeats. While there is no firm evidence that IAs confer the HD phenotype, they are prone to germline CAG repeat instability, particularly repeat expansion when paternally transmitted. Consequently, offspring may inherit a new mutation and develop the disease later in life. Over the last 5 years there has been a renewed interest in IAs. This article provides an overview of the latest research on IAs, including their clinical implications, frequency, haplotype, and likelihood of CAG repeat expansion, as well as patient understanding and current genetic counselling practices. The implications of this growing evidence base for clinical practice are also highlighted. These evidence-based genetic counselling implications may help ensure individuals with an IA predictive test result receive appropriate support, education, and counselling. [ABSTRACT FROM AUTHOR]

Published

2014

3. Large Normal and Intermediate Alleles in the Context of SCA2 Prenatal Diagnosis.

Author

Cruz-Mariño, Tania, Laffita-Mesa, Jose, Gonzalez-Zaldivar, Yanetza, Velazquez-Santos, Miguel, Aguilera-Rodriguez, Raul, Estupinan-Rodriguez, Annelie, Vazquez-Mojena, Yaime, Macleod, Patrick, Paneque, Milena, and Velazquez-Perez, Luis

Abstract

In 2001 a program for predictive testing of Spinocerebellar Ataxia type 2 was developed in Cuba, based on the detection of an abnormal CAG trinucleotide repeat expansion in the ATXN2 gene. A descriptive study was designed to assess the implications of ATXN2 large normal and intermediate alleles in the context of the SCA2 Prenatal Diagnosis Program. Four clinical scenarios were selected based upon the behaviour of large normal and intermediate alleles when passing from one generation to the next, showing expansions, contractions, or stability in the CAG repeat size. In some populations, traditional Mendelian risk figures of 0 % or 50 % may not be applicable due to the high frequency of unstable large normal alleles. Couples with no family history of SCA2 may have a >0 % risk of having an affected offspring. Similarly, couples in which there is both an expanded and a large normal allele may have a recurrence risk >50 %. It is imperative that these issues be addressed with these couples during genetic counseling. These recurrence risks have to be carefully estimated in the presence of such alleles (particularly alleles ≥27 CAG repeats), carriers need to be aware of the potential risk for their descendants, and programs for prenatal diagnosis must be available for them. [ABSTRACT FROM AUTHOR]

Published

2014

4. 'Grasping the Grey': Patient Understanding and Interpretation of an Intermediate Allele Predictive Test Result for Huntington Disease.

Author

Semaka, A., Balneaves, L., and Hayden, M.

Abstract

Since the discovery of the genetic mutation underlying Huntington disease (HD) and the development of predictive testing, the genetics of HD has generally been described as straightforward; an individual receives either mutation-positive or negative predictive test results. However, in actuality, the genetics of HD is complex and a small proportion of individuals receive an unusual predictive test result called an intermediate allele (IA). Unlike mutation-positive or negative results, IAs confer uncertain clinical implications. While individuals with an IA will usually not develop HD, there remains an unknown risk for their children and future generations to develop the disorder. The purpose of this study was to explore how individuals understood and interpreted their IA result. Interviews were conducted with 29 individuals who received an IA result and 8 medical genetics service providers. Interviews were analyzed using the constant comparative method and the coding procedures of grounded theory. Many participants had difficulty ' Grasping the Grey' (i.e. understanding and interpreting their IA results) and their family experience, beliefs, expectations, and genetic counseling influenced the degree of this struggle. The theoretical model developed informs clinical practice regarding IAs, ensuring that this unique subset of patients received appropriate education, support, and counseling. [ABSTRACT FROM AUTHOR]

Published

2013

5. Large normal and reduced penetrance alleles in Huntington disease: instability in families and frequency at the laboratory, at the clinic and in the population.

Author

Sequeiros, J, Ramos, EM, Cerqueira, J, Costa, MC, Sousa, A, Pinto-Basto, J, and Alonso, I

Subjects

*HUNTINGTON disease, *DISEASE prevalence, *GENETIC counseling, *GENOTYPE-environment interaction, *POPULATION genetics, *CLINICAL pathology

Abstract

Sequeiros J, Ramos EM, Cerqueira J, Costa MC, Sousa A, Pinto-Basto J, Alonso I. Large normal and reduced penetrance alleles in Huntington disease: instability in families and frequency at the laboratory, at the clinic and in the population. Large normal (‘intermediate’) alleles may produce de novo expansions in Huntington disease; nevertheless, there is very little evidence about their population prevalence and impact in daily practice, and there are conflicting reports about the extent of their instability. We estimated the frequency of large normal alleles (27–35 CAGs) and of reduced penetrance alleles (36–39 CAGs), as well as the frequency of genotypes carrying them, in (i) a diagnostic laboratory, (ii) a genetic counselling clinic and (iii) the general population. Large normal alleles were present in 6% of a large control sample, 7% of consultands who took pre-symptomatic testing and 7% of samples in the laboratory. Reduced penetrance alleles were found in 1 of 1772 control chromosomes (0.1% of individuals), 5% of 146 pre-symptomatic testees and over 2% of 1214 diagnostic samples (350 families). All 16 alleles sized 27–32 CAGs seemed to be transmitted stably; alleles ≥ 36 repeats were unstable in five families. Seven small full penetrance alleles contracted into the reduced penetrance range, but none into the large normal range. Evidence showed that large normal alleles are relatively frequent and that those with reduced penetrance are not a rare event, either at the laboratory or the clinic. This reinforces the need to understand the genomic context of repeat instability in each family and population. [ABSTRACT FROM AUTHOR]

Published

2010

6. Predictive testing for Huntington disease: interpretation and significance of intermediate alleles.

Author

Semaka, A., Creighton, S., Warby, S., and Hayden, M. R.

Subjects

*HUNTINGTON disease, *RISK assessment, *PSYCHOSOCIAL factors, *GENETIC mutation, *GENEALOGY, *HUMAN sexuality & history, *GENETIC disorders

Abstract

Direct mutation analysis for Huntington disease (HD) became possible in 1993 with the identification of an expanded CAG trinucleotide repeat as the mutation underlying the disease. Expansion of CAG length beyond 35 repeats may be associated with the clinical presentation of HD. HD has never been seen in a person with a CAG size of <36 repeats. Intermediate alleles are defined as being below the affected CAG range but have the potential to expand to >35 CAG repeats within one generation. Thus, children of intermediate allele carriers have a low risk of developing HD. Currently, the intermediate allele range for HD is between 27 and 35 CAG repeats. In this study, we review the current knowledge on intermediate alleles for HD including the CAG repeat range, the intermediate allele frequency, and the clinical implications of an intermediate allele predictive test result. The factors influencing CAG repeat expansion, including the CAG size of the intermediate allele, the sex and age of the transmitting parent, the family history, and the HD gene sequence and haplotype, will also be reviewed. [ABSTRACT FROM AUTHOR]

Published

2006

7. Risk Assessment for Huntington's Disease for (Future) Offspring Requires Offering Preconceptional CAG Analysis to Both Partners

Author

Guido de Wert, Wybo Dondorp, Christine E. M. de Die-Smulders, Aad Tibben, Moniek Losekoot, Emilia K. Bijlsma, Metamedica, RS: CAPHRI - R6 - Promoting Health & Personalised Care, RS: GROW - R4 - Reproductive and Perinatal Medicine, MUMC+: DA KG Polikliniek (9), and Klinische Genetica

Subjects

0301 basic medicine, Male, GUIDELINES, prenatal genetic testing, FAMILIES, 0302 clinical medicine, Trinucleotide Repeats, Pregnancy, Medicine, Predictive testing, preimplantation genetic diagnosis, CAG repeat, education.field_of_study, medicine.diagnostic_test, AGE-OF-ONSET, Obstetrics, ORIGIN, intermediate alleles, REPEAT INSTABILITY, Huntington's disease, Pedigree, REDUCED PENETRANCE ALLELES, Huntington Disease, embryonic structures, Female, Adult, medicine.medical_specialty, preconceptional, Offspring, Genetic counseling, Population, Context (language use), Genetic Counseling, Preimplantation genetic diagnosis, DIAGNOSIS, Risk Assessment, 03 medical and health sciences, Cellular and Molecular Neuroscience, Humans, Genetic Testing, education, Alleles, Genetic testing, HIGH-FREQUENCY, business.industry, partner testing, medicine.disease, GENE, 030104 developmental biology, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Amongst the main reasons people at risk for Huntington's disease (HD) have for undergoing predictive genetic testing are planning a family and prevention of passing on an expanded CAG-repeat to future offspring. After having received an unfavourable test result, a couple may consider prenatal testing in the foetus or preimplantation genetic diagnostic testing (PGD) in embryos. Testing of the foetus or embryos is possible by means of direct testing of the expanded repeat. Optimal reliability in testing the foetus or embryos requires the establishment of the origin of the repeats of both parents in the foetus. For PGD the analysis is combined with or sometimes solely based on identification of the at-risk haplotype in the embryo. This policy implies that in the context of direct testing, the healthy partner's CAG repeat lengths in the HD gene are also tested, but with the expectation that the repeat lengths of the partner are within the normal range, with the proviso that the partner's pedigree is free of clinically confirmed HD. However, recent studies have shown that the expanded repeat has been observed more often in the general population than previously estimated. Moreover, we have unexpectedly observed an expanded repeat in the non-HD partner in four cases which had far-reaching consequences. Hence, we propose that in the context of reproductive genetic counselling, prior to a planned pregnancy, and irrespective of the outcome of the predictive test in the HD-partner, the non-HD partner should also be given the option of being tested on the expanded allele. International recommendations for predictive testing for HD should be adjusted.

Published

2019

8. CAG size-specific risk estimates for intermediate allele repeat instability in Huntington disease

Author

Chris Kay, Jennifer A. Collins, Emilia K. Bijlsma, Michael R. Hayden, Y. Paul Goldberg, Alicia Semaka, Crystal N. Doty, and Fiona Richards

Subjects

Male, Genome instability, congenital, hereditary, and neonatal diseases and abnormalities, Genotype, Biology, Genomic Instability, Germline, Germline mutation, Gene Frequency, mental disorders, New mutations, Genetics, CAG repeat instability, Humans, Allele, Predictive testing, Allele frequency, Alleles, Germ-Line Mutation, Genetics (clinical), Genetic counselling, Huntington disease, Spermatozoa, Intermediate alleles, Trinucleotide Repeat Expansion, Trinucleotide repeat expansion

Abstract

Introduction New mutations for Huntington disease (HD) occur due to CAG repeat instability of intermediate alleles (IA). IAs have between 27 and 35 CAG repeats, a range just below the disease threshold of 36 repeats. While they usually do not confer the HD phenotype, IAs are prone to paternal germline CAG repeat instability. Consequently, they may expand into the HD range upon transmission to the next generation, producing a new mutation. Quantified risk estimates for IA repeat instability are extremely limited but needed to inform clinical practice. Methods Using small-pool PCR of sperm DNA from Caucasian men, we examined the frequency and magnitude of CAG repeat instability across the entire range of intermediate CAG sizes. The CAG size-specific risk estimates generated are based on the largest sample size ever examined, including 30 IAs and 18 198 sperm. Results Our findings demonstrate a significant risk of new mutations. While all intermediate CAG sizes demonstrated repeat expansion into the HD range, alleles with 34 and 35 CAG repeats were associated with the highest risk of a new mutation (2.4% and 21.0%, respectively). IAs with ≥33 CAG repeats showed a dramatic increase in the frequency of instability and a switch towards a preponderance of repeat expansions over contractions. Conclusions These data provide novel insights into the origins of new mutations for HD. The CAG size-specific risk estimates inform clinical practice and provide accurate risk information for persons who receive an IA predictive test result.

Published

2013