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首页> 外文期刊>American Journal of Physiology >Dietary protein regulates hepatic constitutive protein anabolism in rats in a dose-dependent manner and independently of energy nutrient composition.
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Dietary protein regulates hepatic constitutive protein anabolism in rats in a dose-dependent manner and independently of energy nutrient composition.

机译:饮食蛋白以剂量依赖的方式调节大鼠肝脏的组成性蛋白合成代谢,并且与能量营养成分无关。

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We had previously observed that drastic increases in protein consumption greatly modified hepatic protein anabolism in rats, but the confounding effects of other macronutrient changes or a moderate protein increase to generate the same modifications have not yet been established. This study examined the metabolic and hormonal responses of rats subjected to 14-day isoenergetic diets containing normal, intermediate, or high-protein levels (NP: 14% of energy, IP: 33%, HP: 50%) and different carbohydrate (CHO) to fat ratios within each protein level. Fasted or fed rats (n = 104) were killed after the injection of a flooding dose of (13)C-valine. The hepatic protein content increased in line with the dietary protein level (P < 0.05). The hepatic fractional synthesis rates (FSR) of protein were significantly influenced by both the protein level and the nutritional state (fasted vs. fed) (P < 0.0001) but not by the CHO level, reaching on average 110%/day, 92%/day, and 83%/day in rats fed the NP, IP, and HP diets, respectively. The FSR of plasma albumin and muscle did not differ between diets, while feeding tended to increase muscle FSR. Proteolysis, especially the proteasome-dependent system, was down-regulated in the fed state in the liver when protein content increased. Insulin decreased with the CHO level in the diet. Our results reveal that excess dietary protein lowers hepatic constitutive, but not exported, protein synthesis rates, independently of the other macronutrients, and related changes in insulin levels. This response was observed at the moderate levels of protein intake (33%) that are plausible in a context of human consumption.
机译:我们以前曾观察到蛋白质消耗的急剧增加极大地改变了大鼠的肝蛋白质合成代谢,但是尚未确定其他大量营养素变化或蛋白质适度增加以产生相同修饰的混杂效应。这项研究检查了接受14天等能量饮食的老鼠的代谢和激素反应,这些饮食含有正常,中等或高蛋白水平(NP:能量的14%,IP:33%,HP:50%)和不同的碳水化合物(CHO) )与每种蛋白质水平内的脂肪比率。空腹或进食的大鼠(n = 104)在注入泛滥剂量的(13)C-缬氨酸后被杀死。肝蛋白含量随膳食蛋白水平增加而增加(P <0.05)。蛋白质的肝脏分数合成率(FSR)受到蛋白质水平和营养状态的影响(禁食vs.进食)(P <0.0001),但不受CHO水平的影响,平均达到110%/天,达到92%分别以NP,IP和HP饮食喂养的大鼠的每日/天和83%/天。饮食之间血浆白蛋白和肌肉的FSR没有差异,而进食往往会增加肌肉FSR。当蛋白质含量增加时,在肝脏的进食状态下,蛋白水解特别是蛋白酶体依赖性系统被下调。饮食中的胰岛素随CHO水平而降低。我们的研究结果表明,膳食中过量的蛋白质会降低肝脏的组成成分,但不会降低肝脏的蛋白质合成速率,而与其他大量营养素以及胰岛素水平的相关变化无关。在人摄入的情况下合理的蛋白质摄入水平(33%)下观察到了这种反应。

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