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同位素质谱学:一种自上而下的系统生物学方法,用于使用 [1,2-(13)C(2)] 乙酸盐来理解大鼠体内的动态代谢。

Isotopomics: a top-down systems biology approach for understanding dynamic metabolism in rats using [1,2-(13)C(2)] acetate.

机构信息

Nestlé Research Centre, Vers-Chez-les-Blanc, 1000 Lausanne 26, Switzerland.

出版信息

Anal Chem. 2010 Jan 15;82(2):646-53. doi: 10.1021/ac902086g.

DOI:10.1021/ac902086g
PMID:20028023
Abstract

Isotope labeled tracers are commonly used to quantify the turnover rates of various metabolic intermediates and yield information regarding physiological regulation. Studies often only consider either one nutritional state (fasted or fed) and/or one question (e.g., measure of lipid or protein turnover). In this article, we consider a novel application combining the global approach of metabonomics with widespread stable isotope labeling as a way of being able to map metabolism in open mammalian systems, an approach we call "isotopomics". A total of 45 15-week-old male Zucker rats were administrated different amounts (from 0.5 to 8 mmol/kg) of sodium [1,2-(13)C(2)] acetate. Plasma samples taken at 1, 4, and 24 h were analyzed with (13)C nuclear magnetic resonance (NMR) and gas chromatography/mass spectrometry (GC/MS) to measure (13)C isotopic enrichment of 39 plasma metabolites across a wide range of compound classes (amino acids, short-chain fatty acids, lactate, glucose, and free fatty acids). Isotopic enrichment from 0.1-7.1 mole percent excess (MPE) for the highest dose could be reliably measured in 16 metabolites, and the kinetics of their (13)C isotopic enrichment are reported. Clustering metabolites based on (13)C kinetic curves enabled highlighting of time dependent patterns of (13)C distribution through the key metabolic pathways. These kinetic and quantitative data were reported into a biochemical map. This type of isotopomic approach for mapping dynamic metabolism in an open system has great potential for advancing our mechanistic knowledge of how different interventions and diseases can impact the metabolic response of animals and humans.

摘要

同位素标记示踪剂通常用于定量测量各种代谢中间产物的周转率,并提供有关生理调节的信息。研究通常只考虑一种营养状态(禁食或喂食)和/或一个问题(例如,脂质或蛋白质周转率的测量)。在本文中,我们考虑了一种将代谢组学的全局方法与广泛的稳定同位素标记相结合的新应用,以此来能够在开放的哺乳动物系统中绘制代谢图谱,我们称之为“同位素组学”。总共给 45 只 15 周龄雄性 Zucker 大鼠施用不同剂量(0.5 至 8 mmol/kg)的[1,2-(13)C2]乙酸钠。在 1、4 和 24 h 时采集血浆样本,并用(13)C 核磁共振(NMR)和气相色谱/质谱(GC/MS)分析,以测量 39 种血浆代谢物的(13)C 同位素丰度,涵盖了广泛的化合物类别(氨基酸、短链脂肪酸、乳酸盐、葡萄糖和游离脂肪酸)。对于最高剂量,可在 16 种代谢物中可靠地测量到 0.1-7.1 摩尔过量(MPE)的(13)C 同位素丰度,并报告了它们(13)C 同位素丰度的动力学。基于(13)C 动力学曲线对代谢物进行聚类,能够突出关键代谢途径中(13)C 分布的时间依赖性模式。这些动力学和定量数据被报告到生化图谱中。这种在开放系统中绘制动态代谢图谱的同位素组学方法具有很大的潜力,可以提高我们对不同干预措施和疾病如何影响动物和人类代谢反应的机制理解。

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PLoS One. 2019 Oct 28;14(10):e0224297. doi: 10.1371/journal.pone.0224297. eCollection 2019.
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Natural carbon isotope abundance of plasma metabolites and liver tissue differs between diabetic and non-diabetic Zucker diabetic fatty rats.血浆代谢产物和肝组织的天然碳同位素丰度在糖尿病和非糖尿病 Zucker 糖尿病肥胖大鼠之间存在差异。
PLoS One. 2013 Sep 23;8(9):e74866. doi: 10.1371/journal.pone.0074866. eCollection 2013.