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Genetic variation in FADS genes is associated with maternal long-chain PUFA status but not with cognitive development of infants in a high fish-eating observational study

机译:FADS基因的遗传变异与孕妇长链PUFA状况有关但与高食鱼观察研究中的婴儿认知发育无关

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摘要

Long-chain n-6 and n-3 PUFA (LC-PUFA), arachidonic acid (AA) (20:4n-6) and DHA (22:6n-3), are critical for optimal brain development. These fatty acids can be consumed directly from the diet, or synthesized endogenously from precursor PUFA by Δ-5 (encoded by FADS1) and Δ-6 desaturases (encoded by FADS2). The aim of this study was to determine the potential importance of maternal genetic variability in FADS1 and FADS2 genes to maternal LC-PUFA status and infant neurodevelopment in populations with high fish intakes. The Nutrition Cohorts 1 (NC1) and 2 (NC2) are longitudinal observational mother-child cohorts in the Republic of Seychelles. Maternal serum LC-PUFA was measured at 28 weeks gestation and genotyping for rs174537 (FADS1), rs174561 (FADS1), rs3834458 (FADS1-FADS2) and rs174575 (FADS2) was performed in both cohorts. The children completed the Bayley Scales of Infant Development II (BSID-II) at 30 months in NC1 and at 20 months in NC2. Complete data were available for 221 and 1310 mothers from NC1 and NC2 respectively. With increasing number of rs3834458 minor alleles, maternal concentrations of AA were significantly decreased (NC1 p=0.004; NC2 p<0.001) and precursor:product ratios for linoleic acid (LA) (18:2n-6)-to-AA (NC1 p<0.001; NC2 p<0.001) and α-linolenic acid (ALA) (18:3n-3)-to-DHA were increased (NC2 p=0.028). There were no significant associations between maternal FADS genotype and BSID-II scores in either cohort. A trend for improved PDI was found among infants born to mothers with the minor rs3834458 allele. In these high fish-eating cohorts, genetic variability in FADS genes was associated with maternal AA status measured in serum and a subtle association of the FADS genotype was found with neurodevelopment.
机译:长链n-6和n-3 PUFA(LC-PUFA),花生四烯酸(AA)(20:4n-6)和DHA(22:6n-3)对于优化大脑发育至关重要。这些脂肪酸可以直接从饮食中摄取,也可以由前体PUFA通过Δ-5(由FADS1编码)和Δ-6去饱和酶(由FADS2编码)内源合成。这项研究的目的是确定高鱼摄入人群中FADS1和FADS2基因的母亲遗传变异对母亲LC-PUFA状况和婴儿神经发育的潜在重要性。营养队列1(NC1)和营养队列2(NC2)是塞舌尔共和国的纵向观察性母子队列。在孕28周时测量孕妇血清LC-PUFA,并在两个队列中均对rs174537(FADS1),rs174561(FADS1),rs3834458(FADS1-FADS2)和rs174575(FADS2)进行基因分型。这些孩子在NC1的30个月和NC2的20个月时完成了Bayley II婴儿发育量表(BSID-II)。分别有来自NC1和NC2的221位和1310位母亲的完整数据。随着rs3834458次要等位基因数目的增加,孕妇的AA浓度显着降低(NC1 p = 0.004; NC2 p <0.001)以及亚油酸(LA)与AA(NC1)的前体:产物比率p <0.001; NC2 p <0.001)和α-亚麻酸(ALA)(18:3n-3)-DHA升高(NC2 p = 0.028)。在这两个队列中,孕妇FADS基因型与BSID-II评分之间均无显着关联。在具有次要rs3834458等位基因的母亲出生的婴儿中发现了PDI改善的趋势。在这些高食鱼类队列中,FADS基因的遗传变异与血清中测得的母体AA状态相关,并且发现FADS基因型与神经发育之间存在微妙的关联。

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