Song Wenfang, Ren Canqing, Shen Qiuhong, Jiang Yueming, Liu Nan
Shaoxing Publicity and Technical Guidance for Family Planning, Shaoxing 312000, China.
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Zhonghua Yu Fang Yi Xue Za Zhi. 2014 Oct;48(10):900-3.
The effect of the gene polymorphism for the key enzyme's folacin metabolism pathway on plasmatic homocysteine (Hcy) levels in fertile woman was observed.
The subjects were from Shaoxing City, Jiangsu province in 2012, the selection criteria for the women of childbearing age were between 20-45 years old, with an average age of 28.2 (95%CI:27.8-28.6) years old. Sample collection continued uninterrupted lasted seven days, a total of 535 samples were collected, venous blood with EDTA addition or sodium citrate to anticoagulant. After separation, the blood cells and blood plasma were cryopreserved. DNA was extracted using spin column method. All the samples were selected for the gene polymorphism testing of the key enzyme's on folate metabolism and monitoring of plasmatic Hcy level.
Eight single nucleotide polymorphism (SNP) sites of methylenetetrahydrofolate reductase gene (MTHFR) , methionine synthase gene (MS) , synthetic methionine reductase gene (MSR) and cystathionine β synthase gene (CBS) were detected. It was found the genotype AA of the SNP sites-rs1801131 would result higher plasmatic Hcy levels (8.99 µmol/L) than the genotypes CC (7.81 µmol/L) and CA(8.38 µmol/L) (P < 0.01) . Similarly, the genotype TT of the SNP sites-rs1801133 was significantly responded to the increasing of Hcy levels (11.10 µmol/L) than the genotype CC (8.15 µmol/L) and CT (8.45 µmol/L), (P < 0.01) . The two sites of genotype combination of AA-TT could also result in the significant increase of Hcy levels (11.02 µmol/L) than other combined genotypes (genotypes CC-CC, CA-CC, CA-CT, AA-CC, AA-CT), especially the genotype CC-CC. And the risk factor was 1.41 (95CI:1.20-1.66) times over the genotype CC-CC.
The gene mutations of two SNP sites rs1801131 and rs1801133 in MTHFR would increase Hcy levels.
观察叶酸代谢途径关键酶基因多态性对育龄女性血浆同型半胱氨酸(Hcy)水平的影响。
研究对象来自2012年江苏省绍兴市,选择年龄在20 - 45岁之间的育龄女性,平均年龄为28.2岁(95%CI:27.8 - 28.6)。样本采集持续不间断进行7天,共采集535份样本,用添加EDTA或柠檬酸钠的静脉血作为抗凝剂。分离后,血细胞和血浆进行冷冻保存。采用旋转柱法提取DNA。所有样本均进行叶酸代谢关键酶的基因多态性检测及血浆Hcy水平监测。
检测到亚甲基四氢叶酸还原酶基因(MTHFR)、甲硫氨酸合成酶基因(MS)、合成甲硫氨酸还原酶基因(MSR)和胱硫醚β合成酶基因(CBS)的8个单核苷酸多态性(SNP)位点。发现SNP位点rs1801131的AA基因型导致的血浆Hcy水平(8.99 μmol/L)高于CC基因型(7.81 μmol/L)和CA基因型(8.38 μmol/L)(P < 0.01)。同样,SNP位点rs1801133的TT基因型导致的Hcy水平升高(11.10 μmol/L)显著高于CC基因型(8.15 μmol/L)和CT基因型(8.45 μmol/L)(P < 0.01)。AA - TT基因型组合的两个位点导致的Hcy水平(11.02 μmol/L)也显著高于其他组合基因型(CC - CC、CA - CC、CA - CT、AA - CC、AA - CT),尤其是CC - CC基因型。且风险因素是CC - CC基因型的1.41倍(95CI:1.20 - 1.66)。
MTHFR基因中两个SNP位点rs1801131和rs1801133的基因突变会升高Hcy水平。
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