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Effects of omega-3 fatty acid supplementation on the pattern of oxylipins: a short review about the modulation of hydroxy-, dihydroxy-, and epoxy-fatty acids

机译:OMEGA-3脂肪酸补充对氧化素图案的影响:羟基 - ,二羟基 - 和环氧脂肪酸调节的简要述评

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A growing body of evidence suggests that the intake of the long chain omega-3 polyunsaturated fatty acids (n3-PUFA) eicosapentaenoic acid (C20:5 n3, EPA) and docosahexaenoic acid (C22:6 n3, DHA) is linked to beneficial health effects, particularly in the prevention of cardiovascular and inflammatory diseases. Although the molecular mode of action of n3-PUFA is still not fully understood, it is not controversial that a significant portion of the (patho)-physiological effects of PUFA are mediated by their oxidative metabolites, i.e. eicosanoids and other oxylipins. Quantitative targeted oxylipin methods allow the comprehensive monitoring of n3-PUFA supplementation induced changes in the pattern of oxylipins in order to understand their biology. In this short review, results from intervention studies are summarized analyzing >30 oxylipins from different PUFAs in response to n3-PUFA supplementation. The results are not only qualitatively compared with respect to the study design, n3-PUFA dose and trends in the lipid mediators, but also quantitatively based on the relative change in the oxylipin level induced by n3-PUFA. The evaluation of the data from the studies shows that the change in oxylipins generally corresponded to the observed changes in their precursor PUFA, i.e. the lower the individual n3-status at the baseline, the higher the increase in EPA and DHA derived oxylipins. The strongest relative increases were found for EPA derived oxylipins, while changes in arachidonic acid (C20: 4 n6, ARA) derived eicosanoids were heterogeneous. After 3-12 weeks of supplementation, similar relative changes were observed in free and total (free + esterified) oxylipins in plasma and serum. Regarding EPA derived oxylipins, the results indicate a trend for a linear increase with dose. However, the interpretation of the quantitative oxylipin patterns between studies is hampered by strong inter-individual variances in oxylipin levels between and also within the studies. In the future, the reason for these varying oxylipin plasma concentrations needs to be clarified in order to understand oxylipin and n3-PUFA biology.
机译:越来越多的证据表明,摄入长链ω-3多不饱和脂肪酸(N3-PUFA)己二辛醚酸(C20:5 N3,EPA)和二十二碳酸(C22:6 N3,DHA)与有益健康联系起来效果,特别是在预防心血管和炎症疾病中。虽然N3-PUFA的分子作用模式尚未完全理解,但是PUFA的大部分(PATO)型效应的重要部分是由其氧化代谢物介导的,即果香和其他奥基哌嗪。定量靶向氧化素方法允许综合监测N3-PUFA补充诱导的奥氧化物模式变化,以了解他们的生物学。在本次要评审中,干预研究的结果总结了响应于N3-PUFA补充的不同PUFA的> 30个奥氧ipins。结果不仅与研究设计,N3-PUFA剂量和脂质介质中的趋势相比的定性相比,而且还基于N3-PUFA诱导的奥氧化素水平的相对变化。从研究中的数据评估表明,奥氧化物的变化通常对应于其前体PUFA的观察变化,即基线的个体N3状态下降,EPA和DHA衍生的奥氏蛋白的增加越高。对EPA衍生的奥克西普林斯发现了最强的相对增加,而衍生的衍生的果香烷(C20:4 N6,ARA)的变化是非均相的。在补充3-12周后,在血浆和血清中自由和总(自由+酯化)氧化吡汀的相似变化。关于EPA衍生的奥蛋白,结果表明用剂量线性增加的趋势。然而,通过在研究之间的奥氧脂素水平的强烈间差异,研究之间的定量奥克基素模式的解释是阻碍的。在未来,需要澄清这些不同的奥克西素血浆浓度的原因,以了解奥克西宾和N3-PUFA生物学。

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    《Food & Function》 |2017年第7期|共13页
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  • 中图分类 食品工业;
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