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中链甘油三酯富集椰子油与甘草提取物联合对实验性高脂血症小鼠的降脂作用。

Lipid-Lowering Effects of Medium-Chain Triglyceride-Enriched Coconut Oil in Combination with Licorice Extracts in Experimental Hyperlipidemic Mice.

机构信息

Department of Food Science and Nutrition , Hallym University , Chuncheon 24252 , Korea.

Korea Beauty & Health Care Co. , Seoul , Korea.

出版信息

J Agric Food Chem. 2018 Oct 10;66(40):10447-10457. doi: 10.1021/acs.jafc.8b04080. Epub 2018 Oct 2.

DOI:10.1021/acs.jafc.8b04080
PMID:30244576
Abstract

Coconut oil has gained in popularity over recent years as a healthy oil due to its potential cardiovascular benefits. Coconut oil contains medium chain triglycerides (MCT) including lauric acid and capric acid that display beneficial properties in human health. Licorice ( Glycyrrhiza uralensis) is used as a sweetener and in traditional Chinese medicine with anti-inflammatory, antimicrobial, and antioxidant activities. This study investigated the in vivo effects of medium chain-triglycerides (MCT)-coconut oil (MCO) and its combination with licorice extract (LE-MCO) on serum lipid profile, hepatic steatosis, and local fat pad proteins in diet-induced obese mice. No liver toxicity was observed in 45% fat diet (HFD)-fed mice orally treated with LE, MCO, and LE-MCO for 12 weeks. Their supplementation reduced HFD-enhanced body weight, blood glucose, and insulin in mice. Plasma levels of both PLTP and LCAT were boosted in LE-MCO-administered mice. Supplementation of LE-MCO diminished plasma levels of TG and TC with concomitant reduction of the LDL-C level and tended to raise blood HDL-C level compared to that of HFD alone-mice. Treatment of LE-MCO encumbered the hepatic induction of hepatosteatosis-related proteins of SREBP2, SREBP1c, FAS, ACC, and CD36 in HFD-fed mice. Substantial suppression of this induction was also observed in the liver of mice treated with MCO. Oral administration of LE-MCO to HFD mice boosted hepatic activation of AMPK and the induction of UCP-1 and FATP1 in brown fat. Conversely, LE-MCO disturbed hepatic PPAR-LXR-RXR signaling in HFD-fed animals and reversed HFD-elevated epididymal PPARγ. Collectively, oral administration of LE-MCO may impede hyperlipidemia and hepatosteatosis through curtailing hepatic lipid synthesis.

摘要

近年来,由于椰子油具有潜在的心血管益处,因此作为一种健康油而广受欢迎。椰子油含有中链甘油三酯 (MCT),包括月桂酸和己酸,这些酸在人体健康中显示出有益的特性。甘草 (Glycyrrhiza uralensis) 用作甜味剂,并在中国传统医学中具有抗炎、抗菌和抗氧化作用。本研究调查了中链甘油三酯 (MCT)-椰子油 (MCO) 及其与甘草提取物 (LE-MCO) 的组合对饮食诱导肥胖小鼠血清脂质谱、肝脂肪变性和局部脂肪垫蛋白的体内影响。在 45%脂肪饮食 (HFD) 喂养的小鼠中,口服给予 LE、MCO 和 LE-MCO 12 周,未观察到肝毒性。它们的补充减少了 HFD 增强的体重、血糖和胰岛素。LE-MCO 给药小鼠的血浆 PLTP 和 LCAT 水平升高。与单独给予 HFD 的小鼠相比,LE-MCO 的补充减少了 TG 和 TC 的血浆水平,同时降低了 LDL-C 水平,并倾向于提高血液 HDL-C 水平。与单独给予 HFD 的小鼠相比,LE-MCO 处理减少了肝中与肝脂肪变性相关的 SREBP2、SREBP1c、FAS、ACC 和 CD36 蛋白的诱导。在 HFD 喂养的小鼠中,MCO 的治疗也观察到这种诱导的大量抑制。LE-MCO 口服给予 HFD 小鼠可促进棕色脂肪中 AMPK 的肝激活和 UCP-1 和 FATP1 的诱导。相反,LE-MCO 扰乱了 HFD 喂养动物的肝 PPAR-LXR-RXR 信号,并逆转了 HFD 升高的附睾 PPARγ。总之,口服 LE-MCO 可能通过抑制肝脂质合成来阻止高脂血症和肝脂肪变性。

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