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Both maternal and offspring Elovl2 genotypes determine systemic DHA levels in perinatal mice

机译:母本和子代Elovl2基因型都决定围生期小鼠的全身DHA水平

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摘要

The molecular details relevant to dietary supplementation of the omega-3 fatty acid DHA in mothers as well as in their offspring are not clear. The PUFA elongase, elongation of very long-chain fatty acid (ELOVL)2, is a critical enzyme in the formation of DHA in mammals. In order to address the question regarding the origin of DHA during perinatal life, we have used DHA-deficient Elovl2-ablated mice as a model system to analyze the maternal impact on the DHA level in their offspring of various genotypes. Elovl2−/− mothers maintained on control diet had significantly lower systemic levels of DHA compared with the Elovl2+/− and Elovl2+/+ mothers. Dietary DHA administration during the pregnancy and lactation periods led to increased DHA accretion in maternal tissues and serum of all genotypes. The proportion of DHA in the liver and serum of the Elovl2−/− offspring was significantly lower than in the Elovl2+/+ offspring. Remarkably, the DHA level in the Elovl2+/− offspring nursed by DHA-free-fed Elovl2−/− mothers was almost as high as in +/+ pups delivered by +/+ mothers, suggesting that endogenous synthesis in the offspring can compensate for maternal DHA deficiency. Maternal DHA supplementation had a strong impact on offspring hepatic gene expression, especially of the fatty acid transporter, Mfsd2a, suggesting a dynamic interplay between DHA synthesis and DHA uptake in the control of systemic levels in the offspring.
机译:目前尚不清楚与母亲及其后代饮食中补充omega-3脂肪酸DHA有关的分子细节。 PUFA延长酶是非常长链脂肪酸(ELOVL)2的延长,是哺乳动物DHA形成中的关键酶。为了解决有关围产期DHA起源的问题,我们使用了缺乏DHA的Elovl2消融小鼠作为模型系统来分析母体对其各种基因型后代中DHA水平的影响。维持对照饮食的Elovl2 -/-母亲与Elovl2 +/- 和Elovl2 + / + 母亲相比,全身DHA水平明显降低。在妊娠期和哺乳期饮食中施用DHA会导致母体组织和所有基因型血清中DHA的增加。 Elovl2 -/-后代的肝脏和血清中DHA的比例显着低于Elovl2 + / + 后代。值得注意的是,由无DHA喂养的Elovl2 -/-母亲调养的Elovl2 +/- 子代中的DHA含量几乎和+ / +母亲,表明后代的内源性合成可以弥补母亲DHA的缺乏。母体补充DHA对后代肝基因表达,尤其是脂肪酸转运蛋白Mfsd2a的影响很大,表明DHA合成与DHA吸收之间的动态相互作用控制了后代体内的系统水平。

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