Non-disjunction of chromosome 21 in maternal meiosis I: evidence for a maternal age-dependent mechanism involving reduced recombination

Sherman, Stephanie L.; Petersen, Michael B.; Freeman, Sallie B.; Hersey, Jane; Pettay, Dorothy; Taft, Lisa F.; Frantzen, Merete; Mikkelsen, Margareta; Hassold, Terry

doi:10.1093/hmg/3.9.1529

Cited by 148 publications

(114 citation statements)

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“…In contrast, trisomies 18 are not always of maternal origin and are caused, in the majority, by an me2 nondisjunction (reviewed by Jacobs and Hassold 64 ). The implications for UPD16 may be straightforward: the noted frequency of trisomy 16, its unique and constant maternal origin, and the reduced recombination going along with me1-generated disomies 64 should explain the relatively high frequency of UPD16 mat void of isodisomy (reviewed by 20 A somewhat similar commentary could hold true for the UPD's 21 derived from a trisomy 21 where the trend seems as follows: the risk of isodisomy is lowered and the chance of heterodisomy maintained if a lack or a dearth of crossing over recombination is a cause for me1 nondisjunction, as is indeed the case 66 ; such a risk is lessened as well if a (proximal) increase in recombination at me1 favours me2 nondisjunction, which has also been well documented. 67 We see therefore that the mood of chromosome 21, in pathology, is against isodisomic deviancy and does not at all favour the works of 'recessive outlaws'!…”

Section: Upd Types Currently Documentedmentioning

confidence: 92%

A fascination with chromosome rescue in uniparental disomy: Mendelian recessive outlaws and imprinting copyrights infringements

2006

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Section: Upd Types Currently Documentedmentioning

confidence: 92%

A fascination with chromosome rescue in uniparental disomy: Mendelian recessive outlaws and imprinting copyrights infringements

2006

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“…The parents and cell divisions of origin and the reduction in recombination seen in the probands born to the two older mothers are very similar to those seen in a large series of singleton Down syndrome pregnancies. 12 Whilst it is impossible to exclude a genetic predisposition to trisomy 21 non-disjunction in these women, it is an unattractive suggestion because there is no convincing evidence for a genetic predisposition to non-disjunction in our species, either for a specific chromosome 9 or for non-disjunction in general. 14 It therefore seems reasonable to consider that the three trisomic probands in the older women arose by chance.…”

Section: Discussionmentioning

confidence: 84%

“…In the absence of parental mosaicism for a trisomy 21 cell line, the trisomic pregnancies may have arisen either by a nondisjunctional error during meiosis, or by a post-zygotic mitotic error resulting in the gain of a chromosome 21. The majority of trisomy 21 conceptions has been shown to be the result of errors during maternal MI 12 and associated with an increased maternal age at conception.…”

Section: Discussionmentioning

confidence: 99%

Cytogenetic and molecular study of four couples with multiple trisomy 21 pregnancies

et al. 1998

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We studied four families each with three trisomy 21 conceptions. In two of the families the trisomy 21 conceptions all occurred when the mothers were under 35 years of age and in the other two families they all occurred when the mothers were over 35 years of age. Cytogenetic studies showed low level mosaic trisomy 21 in the two younger mothers, but not in the two older. In the three families tested using molecular techniques the results were consistent with the additional chromosome 21 in the trisomic conceptuses being maternally derived. Novel alleles were detected in the trisomic offspring of one of the younger mothers, demonstrating that the mother had been conceived as a trisomy with three different chromosomes 21. Therefore the multiple trisomy 21 pregnancies in the two younger mothers resulted from maternal trisomy 21 mosaicism, but may have been due to chance in the older mothers.

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“…En estos casos, el 75 % se atribuye a la falta de disyunción durante la meiosis I y, el 25 % restante por errores en la meiosis II. La trisomía 21 de origen paterno se ha reportado en 5 % de los casos por errores en la meiosis II (3,4).…”

Section: Polimorfismos De Apoe En El Síndrome De Downunclassified

Polimorfismos del gen ApoE en individuos con síndrome de Down y sus progenitores en una población colombiana

2012

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Introducción. Los polimorfismos en el gen ApoE se han examinado en el síndrome de Down debido a la relación existente de la isoforma E4 con la demencia de tipo Alzheimer que aparece en los individuos con síndrome de Down. Objetivos. Determinar los polimorfismos en el gen ApoE en individuos con síndrome de Down y sus progenitores, y buscar su asociación. Materiales y métodos. Mediante PCR-RFLP, se analizaron los polimorfismos del gen ApoE en 134 individuos jóvenes con síndrome de Down, 87 madres y 54 padres del eje cafetero, y se compararon con una población control de 525 individuos sanos. Resultados. El alelo APOEε3 y el genotipo ε3/ε3 fueron los más frecuentes en todas las poblaciones. La frecuencia alélica de APOEε2 es muy baja y ε2/ε2 está ausente en las poblaciones con síndrome de Down y sus progenitores. El alelo APOEε4 fue más frecuente en individuos con síndrome de Down que en el resto de poblaciones analizadas. Al comparar las frecuencias alélicas y genotípicas entre las poblaciones con síndrome de Down y los progenitores con la población control, mediante la χ 2 de Pearson y los odds ratios por la prueba exacta de Fisher, no se encontraron diferencias estadísticamente significativas. Conclusiones. No se encontró asociación entre los polimorfismos del gen ApoE y el síndrome de Down. Es posible que el tamaño de la muestra o las influencias étnicas hubieran afectado estos resultados. Es necesario hacer otros estudios en poblaciones colombianas y evaluar la asociación con otros genes que se encuentran relacionados con la enfermedad de Alzheimer.Palabras clave: apolipoproteínas E, síndrome de Down, enfermedad de Alzheimer, alelos, genotipo, Colombia. APOE gene polymorphisms associated with Down syndrome in Colombian populationsIntroduction. Gene APOEε4 allele polymorphisms have been examined in Down syndrome because of the relationship between (a) the E4 isoform and (b) the type of Alzheimer's dementia that appears in individuals with Down syndrome. This isoform is considered a risk factor for Alzheimer´s disease development and has been associated with early death in Down syndrome. Objectives. The polymorphisms in the APOE gene were characterized for Down syndrome individuals and their parents, in order to detect associations between the APOE polymorphisms and Down syndrome. Materials and methods. APOE gene polymorphisms were detected by RFLP-PCR and analyzed in 134 young individuals with Down syndrome, 87 mothers and 54 fathers, residents of the departments of Quindío and Risaralda, Colombia. The controls were 525 healthy individuals. Results. The APOEε3 allele and ε3/ε3 genotype were most frequent in all the populations (83-90% and 70-78%). The allelic frequency of APOEε2 was very low and ε2/ε2 (3-7%) was absent in Down syndrome and their parents. The allele APOEε4 was more frequent (11% vs. 9%) in Down syndrome individuals than in the controls. Comparing the allelic and genotypic frequencies between the populations with Down syndrome and their parents with the controls using Pearson χ 2 test and Fisher'...

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Non-disjunction of chromosome 21 in maternal meiosis I: evidence for a maternal age-dependent mechanism involving reduced recombination

Cited by 148 publications

References 0 publications

A fascination with chromosome rescue in uniparental disomy: Mendelian recessive outlaws and imprinting copyrights infringements

A fascination with chromosome rescue in uniparental disomy: Mendelian recessive outlaws and imprinting copyrights infringements

Cytogenetic and molecular study of four couples with multiple trisomy 21 pregnancies

Polimorfismos del gen ApoE en individuos con síndrome de Down y sus progenitores en una población colombiana

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