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口服α-生育酚磷酸酯混合物(TPM)后大鼠体内ω-3(DHA)生物利用度的变化。

Changes in Bioavailability of Omega-3 (DHA) through Alpha-Tocopheryl Phosphate Mixture (TPM) after Oral Administration in Rats.

机构信息

Phosphagenics Limited, Unit A8, 2A Westall Road, Clayton, Melbourne, VIC 3168, Australia.

出版信息

Nutrients. 2017 Sep 20;9(9):1042. doi: 10.3390/nu9091042.

Abstract

Benefits of Omega-3 Docosahexaenoic acid (DHA) supplements are hindered by their poor solubility and bioavailability. This study investigated the bioavailability of various formulations of Omega-3 and tocopheryl phosphate mixture (TPM), following oral administration in rats, and assessed whether TPM could improve the oral absorption of DHA. The rats were administered with a high (265.7 mg/kg) or low dose (88.6 mg/kg) of DHA. TPM was examined at 1:0.1 w/w (low TPM dose) and 1:0.5 w/w (high TPM dose). Over 24 h, the DHA plasma concentration followed a TPM dose-dependent relationship, reflected in the higher mean C values (78.39 and 91.95 μg/mL) and AUC values (1396.60 and 1560.60) for the low and high TPM, respectively. The biggest difference between the low dose DHA control (LDCont) and TPM formulations was at 4 h after supplementation, where the low and high TPM showed a mean 20% (ns) and 50% ( < 0.05) increase in DHA plasma concentrations versus the control formulation. After correcting for baseline endogenous DHA, the mean plasma DHA at 4 h produced by the LD-HTPM was nearly double (90%) the LDC control ( = 0.057). This study demonstrated that co-administering omega-3 with TPM significantly increases the bioavailability of DHA in the plasma, suggesting potential use for commercially available TPM + DHA fortified products.

摘要

ω-3 二十二碳六烯酸(DHA)补充剂的益处受到其较差的溶解度和生物利用度的限制。本研究通过大鼠口服给予各种 ω-3 和生育酚磷酸酯混合物(TPM)制剂,考察了 TPM 对 DHA 口服吸收的改善作用。给大鼠给予高(265.7mg/kg)或低剂量(88.6mg/kg)DHA。考察了 TPM 的 1:0.1 w/w(低 TPM 剂量)和 1:0.5 w/w(高 TPM 剂量)。在 24 小时内,DHA 血浆浓度与 TPM 剂量呈依赖性关系,这反映在低 TPM 和高 TPM 的平均 C 值(分别为 78.39μg/mL 和 91.95μg/mL)和 AUC 值(分别为 1396.60μg/mL 和 1560.60μg/mL)较高。低剂量 DHA 对照组(LDCont)和 TPM 制剂之间最大的差异出现在补充后 4 小时,此时低 TPM 和高 TPM 与对照组相比,DHA 血浆浓度分别增加了 20%(无统计学意义)和 50%(<0.05)。在对基础内源性 DHA 进行校正后,LD-HTPM 在 4 小时产生的平均血浆 DHA 几乎是 LDC 对照组的两倍(=0.057)。本研究表明,与 TPM 联合给予 ω-3 可显著提高 DHA 在血浆中的生物利用度,这表明可用于市售的 TPM+DHA 强化产品。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/21f3/5622802/fca454163b1d/nutrients-09-01042-g001.jpg

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