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Alpha-tocotrienol is the most abundant tocotrienol isomer circulated in plasma and lipoproteins after postprandial tocotrienol-rich vitamin E supplementation

机译:餐后富含维生素E的维生素E补充后,α-生育三烯酚是血浆和脂蛋白中循环最丰富的生育三烯酚异构体

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Background Tocotrienols (T3) and tocopherols (T), both members of the natural vitamin E family have unique biological functions in humans. T3 are detected in circulating human plasma and lipoproteins, although at concentrations significantly lower than α-tocopherol (α-T). T3, especially α-T3 is known to be neuropotective at nanomolar concentrations and this study evaluated the postprandial fate of T3 and α-T in plasma and lipoproteins. Methods Ten healthy volunteers (5 males and 5 females) were administered a single dose of vitamin E [526 mg palm tocotrienol-rich fraction (TRF) or 537 mg α-T] after 7-d pre-conditioning on a T3-free diet. Blood was sampled at baseline (fasted) and 2, 4, 5, 6, 8, and 24 h after supplementation. Concentrations of T and T3 isomers in plasma, triacylglycerol-rich particles (TRP), LDL, and HDL were measured at each postprandial interval. Results After TRF supplementation, plasma α-T3 and γ-T3 peaked at 5 h (α-T3: 4.74 ± 1.69 μM; γ-T3: 2.73 ± 1.27 μM). δ-T3 peaked earlier at 4 h (0.53 ± 0.25 μM). In contrast, α-T peaked at 6 h (30.13 ± 2.91 μM) and 8 h (37.80 ± 3.59 μM) following supplementation with TRF and α-T, respectively. α-T was the major vitamin E isomer detected in plasma, TRP, LDL, and HDL even after supplementation with TRF (composed of 70% T3). No T3 were detected during fasted states. T3 are detected postprandially only after TRF supplementation and concentrations were significantly lower than α-T. Conclusions Bio-discrimination between vitamin E isomers in humans reduces the rate of T3 absorption and affects their incorporation into lipoproteins. Although low absorption of T3 into circulation may impact some of their physiological functions in humans, T3 have biological functions well below concentration noted in this study.
机译:背景天然维生素E家族的生育三烯酚(T3)和生育酚(T)在人类中具有独特的生物学功能。 T3在循环的人血浆和脂蛋白中检测到,尽管其浓度显着低于α-生育酚(α-T)。众所周知,T3,尤其是α-T3在纳摩尔浓度时具有神经保护作用,这项研究评估了血浆和脂蛋白中T3和α-T的餐后命运。方法10名健康志愿者(5名男性和5名女性)在无T3饮食的预处理7天后接受了单剂量维生素E [526 mg棕榈生育三烯酚富集级分(TRF)或537 mgα-T]。 。在基线(禁食)和补充后的2、4、5、6、8和24小时采血。在每个餐后间隔测量血浆,富含三酰基甘油的颗粒(TRP),LDL和HDL中T和T3异构体的浓度。结果补充TRF后,血浆α-T3和γ-T3在5小时达到峰值(α-T3:4.74±1.69μM;γ-T3:2.73±1.27μM)。 δ-T3在4 h(0.53±0.25μM)时达到峰值。相反,补充TRF和α-T后,α-T分别在6 h(30.13±2.91μM)和8 h(37.80±3.59μM)达到峰值。即使补充了TRF(由70%T3组成),α-T仍是血浆,TRP,LDL和HDL中检测到的主要维生素E异构体。禁食状态下未检测到T3。仅在补充TRF后才在餐后检测到T3,并且其浓度显着低于α-T。结论人体内维生素E异构体之间的生物区分会降低T3吸收率,并影响其向脂蛋白中的掺入。尽管T3对循环的低吸收可能会影响其在人体中的某些生理功能,但T3的生物学功能远低于本研究中提到的浓度。

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