Vraneković Jadranka, Božović Ivana Babić, Grubić Zorana, Wagner Jasenka, Pavlinić Dinko, Dahoun Sophie, Bena Frédérique, Culić Vida, Brajenović-Milić Bojana
Department of Biology and Medical Genetics, School of Medicine, University of Rijeka, Rijeka, Croatia.
Genet Test Mol Biomarkers. 2012 Jan;16(1):70-3. doi: 10.1089/gtmb.2011.0066. Epub 2011 Aug 23.
The aims of the present study were to assess (1) the parental origin of trisomy 21 and the stage in which nondisjunction occurs and (2) the relationship between altered genetic recombination and maternal age as risk factors for trisomy 21. The study included 102 cases with Down syndrome from the Croatian population. Genotyping analyses were performed by polymerase chain reaction using 11 short tandem repeat markers along chromosome 21q. The vast majority of trisomy 21 was of maternal origin (93%), followed by paternal (5%) and mitotic origin (2%). The frequencies of maternal meiotic I (MI) and meiotic II errors were 86% and 14%, respectively. The highest proportion of cases with zero recombination was observed among those with maternal MI derived trisomy 21. A higher proportion of telomeric exchanges were presented in cases with maternal MI errors and cases with young mothers, although these findings were not statistically significant. The present study is the first report examining parental origin and altered genetic recombination as a risk factor for trisomy 21 in a Croatian population. The results support that trisomy 21 has a universal genetic etiology across different human populations.
(1)21三体的亲代来源及不分离发生的阶段;(2)作为21三体风险因素的基因重组改变与母亲年龄之间的关系。该研究纳入了来自克罗地亚人群的102例唐氏综合征病例。采用聚合酶链反应,利用21号染色体长臂上的11个短串联重复序列标记进行基因分型分析。绝大多数21三体源于母亲(93%),其次是父亲(5%)和有丝分裂来源(2%)。母亲减数分裂I(MI)和减数分裂II错误的频率分别为86%和14%。在源于母亲MI的21三体病例中,观察到重组为零的病例比例最高。在母亲MI错误的病例和母亲年龄较小的病例中,端粒交换的比例较高,尽管这些发现无统计学意义。本研究是首篇在克罗地亚人群中探讨21三体的亲代来源及基因重组改变作为风险因素的报告。结果支持21三体在不同人群中具有普遍的遗传病因。
