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首页> 外文期刊>Regulatory Toxicology and Pharmacology: RTP >The safety of the use of ethyl oleate in food is supported by metabolism data in rats and clinical safety data in humans.
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The safety of the use of ethyl oleate in food is supported by metabolism data in rats and clinical safety data in humans.

机译:大鼠的新陈代谢数据和人体的临床安全性数据支持了在食品中使用油酸乙酯的安全性。

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The absorption, distribution, and excretion of radiolabeled ethyl oleate (EO) was studied in Sprague-Dawley rats after a single, peroral dose of 1.7 or 3.4g/kg body weight and was compared with a radiolabeled triacylglycerol (TG) containing only oleic acid as the fatty acid (triolein). Both test materials were well absorbed with approximately 70-90% of the EO dose absorbed and approximately 90-100% of the TG dose absorbed. At sacrifice (72h post-dose), tissue distribution of EO-derived radioactivity and TG-derived radioactivity was similar. The tissue with the highest concentration of radioactivity in both groups was mesenteric fat. The other organs and tissues had very low concentrations of test material-derived radioactivity. Both test materials were rapidly and extensively excreted as CO(2) with no remarkable differences between their excretion profiles. Approximately 40-70% of the administered dose for both groups was excreted as CO(2) within the first 12h (consistent with beta-oxidation of fatty acids). Fecal elimination of EO appeared to be dose-dependent. At the dose of 1.7g/kg, 7-8% of the administered dose was eliminated in the feces. At the dose of 3.4g/kg, approximately 20% of the administered dose was excreted in the feces. Excretion of TG-derived radiolabel in the feces was approximately 2-4% for both doses. Overall, the results demonstrate that the absorption, distribution, and excretion of radiolabeled EO is similar to that of TG providing evidence that the oleic acid moiety of EO is utilized in the body as a normal dietary TG-derived fatty acid. To confirm the expected safety of EO in humans, a total of 235 subjects participated in a 12-week trial where two levels of ethyl oleate in a milk-based beverage were investigated: 8g/day in a single serving (approximately 0.1g/kg) and 16g/day taken in two divided servings (approximately 0.2g/kg). Adverse events (AEs) were recorded throughout the 12-week trial. In addition, a brief physical exam (including vital signs and body weight), ECGs, fasting serum chemistry profile, serum lipid profile, and urinalysis were performed at baseline and after study completion. Results showed the incidence of reported AEs was similar between the EO groups and the control groups. Analysis of comprehensive laboratory data revealed no EO exposure-related, clinically significant adverse changes in laboratory parameters. These studies demonstrated that EO has a highly favorable safety profile and is well tolerated in the diet.
机译:在单次口服剂量为1.7或3.4g / kg体重后,在Sprague-Dawley大鼠中研究了放射性标记的油酸乙酯(EO)的吸收,分布和排泄,并将其与仅含油酸的放射性标记的三酰基甘油(TG)进行了比较。作为脂肪酸(三油精)。两种测试材料均被良好吸收,吸收了大约70-90%的EO剂量,吸收了大约90-100%的TG。处死后(给药后72小时),EO衍生放射性和TG衍生放射性的组织分布相似。两组中放射性浓度最高的组织是肠系膜脂肪。其他器官和组织的受试物质来源的放射性浓度非常低。两种测试材料都作为CO(2)迅速而广泛地排泄,其排泄曲线之间没有显着差异。两组的大约40-70%的给药剂量在头12小时内以CO(2)的形式排出(与脂肪酸的β-氧化一致)。粪便消除EO似乎是剂量依赖性的。在1.7g / kg的剂量下,粪便中7-8%的剂量被清除。以3.4g / kg的剂量,大约20%的给药剂量排泄在粪便中。对于两种剂量,粪便中TG衍生的放射性标记的排泄率约为2-4%。总体而言,结果表明放射性标记的EO的吸收,分布和排泄与TG相似,这提供了EO的油酸部分作为正常饮食中TG衍生的脂肪酸在体内被利用的证据。为了确认EO对人体的预期安全性,共有235名受试者参加了为期12周的试验,研究了乳基饮料中两种油酸乙酯的含量:单次8克/天(约0.1克/千克) )和16克/天,分为两份(约0.2克/千克)。在整个12周的试验中记录了不良事件(AE)。此外,在基线和研究完成后进行了简短的体格检查(包括生命体征和体重),ECG,空腹血清化学概况,血清脂质概况和尿液分析。结果显示,EO组和对照组之间报告的AE发生率相似。对综合实验室数据的分析表明,实验室参数没有与EO暴露相关的临床显着不利变化。这些研究表明,EO具有高度有利的安全性,并且在饮食中具有良好的耐受性。

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