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一项针对成年斯普拉格-道利大鼠的¹⁴C-亮氨酸吸收、分布、代谢及排泄(ADME)研究显示,β-羟基-β-甲基丁酸是一种代谢产物。

A (14)C-leucine absorption, distribution, metabolism and excretion (ADME) study in adult Sprague-Dawley rat reveals β-hydroxy-β-methylbutyrate as a metabolite.

作者信息

Lee Anthony J, Beno David W A, Zhang Xiaolin, Shapiro Robin, Mason Mark, Mason-Bright Tanita, Surber Bruce, Edens Neilé K

机构信息

Drug Metabolism and Pharmacokinetics, AbbVie Inc., 1 North Waukegan Road, North Chicago, IL, 60064, USA.

出版信息

Amino Acids. 2015 May;47(5):917-24. doi: 10.1007/s00726-015-1920-6. Epub 2015 Jan 25.

Abstract

Leucine is an essential branched-chain amino acid that acts as a substrate for protein synthesis and as a signaling molecule. Leucine not incorporated into muscle protein is ultimately oxidized through intermediates such as β-hydroxy-β-methylbutyrate (HMB) which itself is reported to enhance muscle mass and function in rats and humans. HMB has been reported in the plasma following oral leucine administration in sheep and pigs but not in Sprague-Dawley rats, the standard preclinical model. Therefore, we conducted radiolabeled absorption, distribution, metabolism and excretion (ADME) studies in rats using a low (3 mg/kg) or high dose (1,000 mg/kg) of (14)C-leucine. Blood, tissue, and urine samples were analyzed for (14)C-leucine and its metabolites by HPLC-MS. Our results show for the first time that (14)C-HMB appears in plasma and urine of rats following an oral dose of (14)C-leucine. (14)C-leucine appears in plasma as (14)C-α-ketoisocaproic acid (KIC) with a slower time course than (14)C-HMB, a putative product of KIC. Further, two novel metabolites of leucine were detected in urine, N-acetyl leucine and glycyl leucine. Mass balance studies demonstrate that excretory routes accounted for no more than 0.9 % of the radiolabel and approximately 61 % of the dose was recovered in the carcass. Approximately 65 % of the dose was recovered in total, suggesting that approximately one-third of the leucine dose is oxidized to CO2. In conclusion, this study demonstrates endogenous production of HMB from leucine in adult rats, a standard preclinical model used to guide design of clinical trials in nutrition.

摘要

亮氨酸是一种必需的支链氨基酸,它作为蛋白质合成的底物以及信号分子发挥作用。未掺入肌肉蛋白质的亮氨酸最终会通过诸如β-羟基-β-甲基丁酸酯(HMB)等中间体被氧化,据报道,HMB本身可增加大鼠和人类的肌肉质量并改善肌肉功能。在绵羊和猪口服亮氨酸后,血浆中已检测到HMB,但在标准临床前模型——斯普拉格-道利大鼠中未检测到。因此,我们使用低剂量(3 mg/kg)或高剂量(1000 mg/kg)的(14)C-亮氨酸对大鼠进行了放射性标记吸收、分布、代谢和排泄(ADME)研究。通过HPLC-MS分析血液、组织和尿液样本中的(14)C-亮氨酸及其代谢产物。我们的结果首次表明,口服(14)C-亮氨酸后,大鼠的血浆和尿液中出现了(14)C-HMB。(14)C-亮氨酸以(14)C-α-酮异己酸(KIC)的形式出现在血浆中,其时间进程比KIC的假定产物(14)C-HMB要慢。此外,在尿液中检测到了亮氨酸的两种新代谢产物,N-乙酰亮氨酸和甘氨酰亮氨酸。质量平衡研究表明,排泄途径占放射性标记的比例不超过0.9%,约61%的剂量在胴体中回收。总计约65%的剂量被回收,这表明约三分之一的亮氨酸剂量被氧化为二氧化碳。总之,本研究证明了在成年大鼠(一种用于指导营养临床试验设计的标准临床前模型)中,亮氨酸可内源性产生HMB。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c95e/4412734/9efc2fd884bf/726_2015_1920_Fig1_HTML.jpg

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