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基于 NMR 的代谢组学和呼吸研究显示,在低剂量慢性 T(1)AM 治疗期间会发生脂质和蛋白质分解代谢。

NMR-based metabolomics and breath studies show lipid and protein catabolism during low dose chronic T(1)AM treatment.

机构信息

Department of Zoology, University of Wisconsin-Madison, Madison, Wisconsin, USA.

出版信息

Obesity (Silver Spring). 2013 Dec;21(12):2538-44. doi: 10.1002/oby.20391. Epub 2013 May 29.

Abstract

OBJECTIVE

3-Iodothyronamine (T1 AM), an analog of thyroid hormone, is a recently discovered fast-acting endogenous metabolite. Single high-dose treatments of T1 AM have produced rapid short-term effects, including a reduction of body temperature, bradycardia, and hyperglycemia in mice.

DESIGN AND METHODS

The effect of daily low doses of T1 AM (10 mg/kg) for 8 days on weight loss and metabolism in spontaneously overweight mice was monitored. The experiments were repeated twice (n = 4). Nuclear magnetic resonance (NMR) spectroscopy of plasma and real-time analysis of exhaled (13) CO2 in breath by cavity ring down spectroscopy (CRDS) were used to detect T1 AM-induced lipolysis.

RESULTS

CRDS detected increased lipolysis in breath shortly after T1 AM administration that was associated with a significant weight loss but independent of food consumption. NMR spectroscopy revealed alterations in key metabolites in serum: valine, glycine, and 3-hydroxybutyrate, suggesting that the subchronic effects of T1 AM include both lipolysis and protein breakdown. After discontinuation of T1 AM treatment, mice regained only 1.8% of the lost weight in the following 2 weeks, indicating lasting effects of T1 AM on weight maintenance.

CONCLUSIONS

CRDS in combination with NMR and (13) C-metabolic tracing constitute a powerful method of investigation in obesity studies for identifying in vivo biochemical pathway shifts and unanticipated debilitating side effects.

摘要

目的

3-碘甲状腺原氨酸(T1 AM)是一种甲状腺激素类似物,是最近发现的一种快速作用的内源性代谢物。单次高剂量的 T1 AM 治疗可产生快速的短期效应,包括降低小鼠的体温、心率和血糖。

设计和方法

监测每日低剂量 T1 AM(10mg/kg)连续 8 天对自发性超重小鼠体重减轻和代谢的影响。实验重复两次(n=4)。通过腔衰减光谱(CRDS)检测呼出的(13)CO2的实时分析和血浆的核磁共振(NMR)光谱来检测 T1 AM 诱导的脂肪分解。

结果

CRDS 检测到 T1 AM 给药后不久呼吸中的脂肪分解增加,这与显著的体重减轻有关,但与食物消耗无关。NMR 光谱显示血清中关键代谢物的改变:缬氨酸、甘氨酸和 3-羟基丁酸,表明 T1 AM 的亚慢性作用包括脂肪分解和蛋白质分解。停止 T1 AM 治疗后,小鼠在接下来的 2 周内仅恢复了失去体重的 1.8%,表明 T1 AM 对体重维持有持久的影响。

结论

CRDS 与 NMR 和(13)C 代谢示踪相结合,构成了肥胖研究中识别体内生化途径变化和意外衰弱副作用的强大方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b3e/3692609/30a2cd7e2da5/nihms436313f1.jpg

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