ABNORMAL FOLATE METABOLISM;
GENETIC POLYMORPHISMS;
COMMON MUTATION;
HIGH PREVALENCE;
MTHFR;
HOMOCYSTEINE;
DNA;
PATHWAY;
DISEASE;
ASSOCIATION;
D O I:
10.1089/gtmb.2010.0057
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
Background: The activity of the methylenetetrahydrofolate reductase (MTHFR) enzyme is regulated by the two polymorphisms C677T and A1298C, which reduce enzyme activity and result in hypomethylation of chromosomes that increase the risk of nondisjunction. These polymorphisms are suggested to be risk factors for Down syndrome (DS) in some populations. Aim: The aim of this study was to test if C677T and A1298C polymorphisms are correlated to maternal risk of DS in Jordan. Methods: The proportions of C677T and A1298C polymorphisms were examined in 53 case mothers who delivered DS children and 29 controls. The median age of case mothers was 35 years when delivering their affected children. Polymerase chain reaction-restriction fragment length polymorphism was used for genotyping. Results: The frequency of MTHFR C677T allele in all DS mothers was 3.2-fold higher than in the controls (odds ratio [OR] = 3.12, 95% confidence interval [CI]: 1.303-7.677). Also, the proportion of 677T in the older case mothers was different from the controls, but was significantly higher in younger case mothers than in the controls (OR = 4.2, 95% CI: 1.61-10.97, p = 0.003). The proportions of 677CT and 677TT genotypes in younger cases are, respectively, 10- and 9-fold higher than in the controls. The proportions of MTHFR A1298C are significantly different among all case groups and the controls (chi(2) - 4.27, p - 0.127), but there was a significant difference between young case mothers and both older case mothers group and the controls (OR - 1.25, 95% CI: 0.405-3.85, p - 0.698). Conclusions: There is strong association between MTHFRC677T and maternal risk of DS in Jordanian mothers younger than 35 years old and the MTHFR1298C allele has a lesser but additive risk effect in MTHFR677T/1298C compound heterozygotes.
机构:
Benemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico
Meneses-Sanchez, Perla
Garcia-Hernandez, Samantha C.
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Benemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico
Garcia-Hernandez, Samantha C.
Porchia, Leonardo M.
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IMSS, Ctr Invest Biomed Oriente, Lab Invest Fisiopatol Enfermedades Cron, Km 4-5 Carretera Fed Atlixco Metepec, Puebla 42730, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico
Porchia, Leonardo M.
Perez-Fuentesz, Ricardo
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IMSS, Ctr Invest Biomed Oriente, Lab Invest Fisiopatol Enfermedades Cron, Km 4-5 Carretera Fed Atlixco Metepec, Puebla 42730, Mexico
Benemerita Univ Autonoma Puebla, Fac Med, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico
Perez-Fuentesz, Ricardo
Torres-Rasgado, Enrique
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Benemerita Univ Autonoma Puebla, Fac Med, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico
Torres-Rasgado, Enrique
Del Angel Soto, Alejandra
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Benemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico
Del Angel Soto, Alejandra
Elba Gonzalez-Mejia, M.
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Benemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, MexicoBenemerita Univ Autonoma Puebla, Fac Med, Dept Genet, 13 Sur 2901 Col Volcanes, Puebla 72420, Pue, Mexico