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叶酸代谢途径多态性与营养缺乏相结合作为唐氏综合征的母体易感因素的影响。

The impact of folate pathway polymorphisms combined to nutritional deficiency as a maternal predisposition factor for Down syndrome.

作者信息

Santos-Rebouças C B, Corrêa J C, Bonomo A, Fintelman-Rodrigues N, Moura K C V, Rodrigues C S C, Santos J M, Pimentel M M G

机构信息

Departamento de Genética, Universidade do Estado do Rio de Janeiro, Instituto de Biologia Alcântara Gomes, Serviço de Genética, Rio de Janeiro, RJ, Brazil.

出版信息

Dis Markers. 2008;25(3):149-57. doi: 10.1155/2008/487023.

Abstract

Polymorphisms in genes encoding folate metabolizing enzymes have been linked to an increased risk of maternal chromosomal nondisjunction in several populations. With the purpose of evaluating this relationship, we compared the frequencies of 677C>T and 1298A>C polymorphisms in the methylenetetrahydrofolate reductase gene (MTHFR) and 66A>G in the methionine synthase reductase gene (MTRR) between 103 young mothers of Down syndrome (DS) individuals and 108 control mothers, whose offspring was karyotypically normal, correlating it with an estimative of folate and - related micronutrients levels intake. Maternal and paternal transmission frequencies of MTHFR 677T allele were also examined to access potential parent-of-origin effects. PCR-RFLP for genomic DNA was accomplished and allele/genotype frequencies differences were determined using the x(2) test, whereas pattern of transmission of the MTHFR 677 allele was analyzed by transmission disequilibrium test. None of the polymorphisms seemed to be more frequent in case mothers than in controls, either individually or combined. The estimative of nutritional intake revealed that folate consumption median was inadequate in both groups, whereas methionine and zinc consumption medians were significantly greater in control mothers. It suggests that such interaction between genetic profile and environment could predispose this sub group of women to have a DS child. Additional studies focusing the interaction between nutritional intakes, biochemical data and folate pathway polymorphisms are needed to confirm the present results. The possibility of neutralize the biochemical negative effects of folate-related polymorphisms through oral supplementation could provide new targets for DS prevention.

摘要

在几个群体中,编码叶酸代谢酶的基因多态性与母亲染色体不分离风险增加有关。为了评估这种关系,我们比较了103名唐氏综合征(DS)患儿的年轻母亲和108名对照母亲(其后代核型正常)中,亚甲基四氢叶酸还原酶基因(MTHFR)的677C>T和1298A>C多态性以及甲硫氨酸合成酶还原酶基因(MTRR)的66A>G多态性的频率,并将其与叶酸及相关微量营养素水平摄入量的估计值相关联。还检查了MTHFR 677T等位基因的母系和父系传递频率,以了解潜在的亲本来源效应。完成了基因组DNA的PCR-RFLP分析,并使用x(2)检验确定等位基因/基因型频率差异,而通过传递不平衡检验分析MTHFR 677等位基因的传递模式。无论是单独还是组合,病例母亲中似乎没有一种多态性比对照组更常见。营养摄入量的估计显示,两组的叶酸摄入量中位数均不足,而对照母亲的甲硫氨酸和锌摄入量中位数显著更高。这表明这种基因谱与环境之间的相互作用可能使这一亚组女性易生出患有唐氏综合征的孩子。需要进行更多关注营养摄入、生化数据和叶酸途径多态性之间相互作用的研究来证实目前的结果。通过口服补充剂中和叶酸相关多态性的生化负面影响的可能性,可能为唐氏综合征的预防提供新的靶点。

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