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长期使用胍丁胺对分子和代谢的影响。

The molecular and metabolic influence of long term agmatine consumption.

机构信息

From the Children's Hospital of Philadelphia.

出版信息

J Biol Chem. 2014 Apr 4;289(14):9710-29. doi: 10.1074/jbc.M113.544726. Epub 2014 Feb 12.

Abstract

Agmatine (AGM), a product of arginine decarboxylation, influences multiple physiologic and metabolic functions. However, the mechanism(s) of action, the impact on whole body gene expression and metabolic pathways, and the potential benefits and risks of long term AGM consumption are still a mystery. Here, we scrutinized the impact of AGM on whole body metabolic profiling and gene expression and assessed a plausible mechanism(s) of AGM action. Studies were performed in rats fed a high fat diet or standard chow. AGM was added to drinking water for 4 or 8 weeks. We used (13)C or (15)N tracers to assess metabolic reactions and fluxes and real time quantitative PCR to determine gene expression. The results demonstrate that AGM elevated the synthesis and tissue level of cAMP. Subsequently, AGM had a widespread impact on gene expression and metabolic profiling including (a) activation of peroxisomal proliferator-activated receptor-α and its coactivator, PGC1α, and (b) increased expression of peroxisomal proliferator-activated receptor-γ and genes regulating thermogenesis, gluconeogenesis, and carnitine biosynthesis and transport. The changes in gene expression were coupled with improved tissue and systemic levels of carnitine and short chain acylcarnitine, increased β-oxidation but diminished incomplete fatty acid oxidation, decreased fat but increased protein mass, and increased hepatic ureagenesis and gluconeogenesis but decreased glycolysis. These metabolic changes were coupled with reduced weight gain and a curtailment of the hormonal and metabolic derangements associated with high fat diet-induced obesity. The findings suggest that AGM elevated the synthesis and levels of cAMP, thereby mimicking the effects of caloric restriction with respect to metabolic reprogramming.

摘要

胍丁胺(AGM)是精氨酸脱羧产物,影响多种生理和代谢功能。然而,其作用机制、对全身基因表达和代谢途径的影响以及长期 AGM 消耗的潜在益处和风险仍然是一个谜。在这里,我们仔细研究了 AGM 对全身代谢谱和基因表达的影响,并评估了 AGM 作用的可能机制。研究在高脂肪饮食或标准饲料喂养的大鼠中进行。AGM 添加到饮用水中 4 或 8 周。我们使用(13)C 或(15)N 示踪剂来评估代谢反应和通量,并使用实时定量 PCR 来确定基因表达。结果表明,AGM 升高了 cAMP 的合成和组织水平。随后,AGM 对基因表达和代谢谱产生了广泛影响,包括(a)激活过氧化物酶体增殖物激活受体-α及其共激活因子 PGC1α,以及(b)增加过氧化物酶体增殖物激活受体-γ 和调节糖异生、生酮作用和肉碱生物合成和转运的基因表达。基因表达的变化与组织和全身肉碱和短链酰基肉碱水平的提高、β-氧化增加但不完全脂肪酸氧化减少、脂肪减少但蛋白质质量增加以及肝尿素生成和糖异生增加但糖酵解减少有关。这些代谢变化伴随着体重增加减少以及与高脂肪饮食诱导肥胖相关的激素和代谢紊乱的减少。研究结果表明,AGM 升高了 cAMP 的合成和水平,从而在代谢重编程方面模拟了热量限制的作用。

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