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Significance of dietary folate intake, homocysteine levels and MTHFR 677 C>T genotyping in South African patients diagnosed with depression: Test development for clinical application

机译:南非确诊患有抑郁症的患者的饮食中叶酸摄入量,高半胱氨酸水平和MTHFR 677 C> T基因分型的意义:临床应用试验开发

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Low folate intake in the presence of the functional MTHFR 677 C > T (rs1801133) polymorphism is an important cause of elevated homocysteine levels previously implicated in major depressive disorder (MDD) and many other chronic diseases. In this study the clinical relevance and inter-relationship of these aspects were evaluated in 86 South African patients diagnosed with MDD and 97 population-matched controls participating in a chronic diseases screening program. A questionnaire-based clinical and nutrition assessment was performed, homocysteine levels determined, and all study participants genotyped for MTHFR 677 C > T (rs1801133) using allele-specific TaqMan technology. The folate score was found to be significantly lower in the patient group compared to controls (p=0.003) and correlated with increased body mass index (BMI), particularly in females with MDD (p=0.009). BMI was significantly higher in the MDD patients compared with controls after adjustment for age and sex (p=0.015), but this association was no longer significant after further adjustment for the level of folate intake in the diet. In MDD patients but not controls, the minor T-allele of MTHFR 677 C > T was associated with increased BMI (p=0.032), which in turn correlated significantly with increased homocysteine levels. The significant association between BMI and homocysteine levels was observed in both the MDD patient (p=0.049) and control (p=0.018) study groups. The significantly higher homocysteine levels observed in MDD patients compared to controls after adjustment for age and sex (p=0.030), therefore appears to be mediated by the effects of MTHFR 677 C > T and low folate intake on BMI. Detection of the low-penetrance MTHFR 677 C > T mutation reinforces the importance of folate intake above the recommended daily dose to prevent or restore dysfunction of the methylation pathway.
机译:功能性MTHFR 677 C> T(rs1801133)多态性存在时叶酸摄入量低是高半胱氨酸水平升高的重要原因,以前该水平与主要抑郁症(MDD)和许多其他慢性疾病有关。在这项研究中,评估了86例诊断为MDD的南非患者和97名参与慢性疾病筛查程序的人群匹配对照的这些方面的临床相关性和相互关系。进行了基于问卷的临床和营养评估,确定了同型半胱氨酸水平,并使用等位基因特异性TaqMan技术对所有研究参与者进行了MTHFR 677 C> T(rs1801133)基因分型。与对照组相比,患者组的叶酸评分显着降低(p = 0.003),并且与体重指数(BMI)增加相关,特别是在患有MDD的女性中(p = 0.009)。调整年龄和性别后,MDD患者的BMI显着高于对照组(p = 0.015),但在进一步调整饮食中叶酸摄入水平后,这种关联不再显着。在MDD患者而非对照组中,MTHFR 677 C> T的次要T等位基因与BMI升高相关(p = 0.032),而BMI与高半胱氨酸水平显着相关。在MDD患者(p = 0.049)和对照组(p = 0.018)的研究组中均观察到BMI与同型半胱氨酸水平之间的显着相关性。在调整了年龄和性别之后,与对照组相比,MDD患者中观察到的同型半胱氨酸水平明显更高(p = 0.030),因此似乎是由MTHFR 677 C> T和低叶酸摄入对BMI的影响所介导的。低渗透性MTHFR 677 C> T突变的检测加强了叶酸摄入量高于建议的每日剂量的重要性,以预防或恢复甲基化途径的功能障碍。

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