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乳清蛋白分离物可抵抗高脂肪饮食对能量摄入和与能量平衡相关基因在下丘脑和脂肪组织中表达的影响。

Whey protein isolate counteracts the effects of a high-fat diet on energy intake and hypothalamic and adipose tissue expression of energy balance-related genes.

机构信息

Teagasc Food Research Centre, Moorepark, Fermoy, County Cork, Republic of Ireland.

出版信息

Br J Nutr. 2013 Dec 14;110(11):2114-26. doi: 10.1017/S0007114513001396. Epub 2013 Jun 4.

Abstract

The intake of whey protein isolate (WPI) is known to reduce high-fat diet (HFD)-induced body-weight gain and adiposity. However, the molecular mechanisms are not fully understood. To this end, we fed C57BL/6J mice for 8 weeks with diets containing 10 % energy as fat (low-fat diet, LFD) or 45 % energy as fat (HFD) enriched with either 20 % energy as casein (LFD and HFD) or WPI (high-fat WPI). Metabolic parameters and the hypothalamic and epididymal adipose tissue expression of energy balance-related genes were investigated. The HFD increased fat mass and plasma leptin levels and decreased the dark-phase energy intake, meal number, RER, and metabolic (VO₂ and heat) and locomotor activities compared with the LFD. The HFD increased the hypothalamic tissue mRNA expression of the leptin receptor, insulin receptor (INSR) and carnitine palmitoyltransferase 1b (CPT1b). The HFD also reduced the adipose tissue mRNA expression of GLUT4 and INSR. In contrast, WPI reduced fat mass, normalised dark-phase energy intake and increased meal size in HFD-fed mice. The dietary protein did not have an impact on plasma leptin, insulin, glucose or glucagon-like peptide 1 levels, but increased plasma TAG levels in HFD-fed mice. At a cellular level, WPI significantly reduced the HFD-associated increase in the hypothalamic tissue mRNA expression of the leptin receptor, INSR and CPT1b. Also, WPI prevented the HFD-induced reduction in the adipose tissue mRNA expression of INSR and GLUT4. In comparison with casein, the effects of WPI on energy intake and hypothalamic and adipose tissue gene expression may thus represent a state of reduced susceptibility to weight gain on a HFD.

摘要

乳清蛋白分离物(WPI)的摄入已知可减少高脂肪饮食(HFD)引起的体重增加和肥胖。然而,其分子机制尚不完全清楚。为此,我们用含有 10%能量脂肪的饮食(低脂饮食,LFD)或含有 45%能量脂肪的饮食(HFD)喂养 C57BL/6J 小鼠 8 周,这些饮食分别用 20%能量的乳清蛋白(LFD 和 HFD)或 WPI(高脂肪 WPI)富集。研究了代谢参数以及下丘脑和附睾脂肪组织中与能量平衡相关的基因表达。与 LFD 相比,HFD 增加了脂肪量和血浆瘦素水平,并降低了暗期能量摄入、进餐次数、呼吸商和代谢(VO₂ 和热量)以及运动活动。HFD 增加了下丘脑组织中瘦素受体、胰岛素受体(INSR)和肉碱棕榈酰转移酶 1b(CPT1b)的 mRNA 表达。HFD 还降低了脂肪组织中 GLUT4 和 INSR 的 mRNA 表达。相比之下,WPI 减少了 HFD 喂养小鼠的脂肪量,使暗期能量摄入正常化,并增加了进餐量。饮食蛋白对血浆瘦素、胰岛素、葡萄糖或胰高血糖素样肽 1 水平没有影响,但增加了 HFD 喂养小鼠的血浆 TAG 水平。在细胞水平上,WPI 显著降低了 HFD 引起的下丘脑组织中瘦素受体、INSR 和 CPT1b 的 mRNA 表达增加。此外,WPI 防止了 HFD 诱导的脂肪组织中 INSR 和 GLUT4 的 mRNA 表达减少。与乳清蛋白相比,WPI 对能量摄入以及下丘脑和脂肪组织基因表达的影响可能代表了对 HFD 体重增加的敏感性降低的状态。

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