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首页> 外文期刊>Physiological genomics >A combined H-1-NMR spectroscopy- and mass spectrometry-based metabolomic study of the PPAR-alpha null mutant mouse defines profound systemic changes in metabolism linked to the metabolic syndrome
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A combined H-1-NMR spectroscopy- and mass spectrometry-based metabolomic study of the PPAR-alpha null mutant mouse defines profound systemic changes in metabolism linked to the metabolic syndrome

机译:基于H-1-NMR和质谱的结合代谢组学研究的PPAR-alpha null突变小鼠定义了与代谢综合征相关的新陈代谢的深刻系统性变化

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摘要

A combined H-1-NMR spectroscopy- and mass spectrometry-based metabolomic study of the PPAR-alpha null mutant mouse defines profound systemic changes in metabolism linked to the metabolic syndrome. Physiol Genomics 27: 178-186, 2006. First published July 25, 2006; doi:10.1152/physiolgenomics. 00060.2006.-The mobilization of triacylglycerides from storage in adipocytes to the liver is a vital response to the fasting state in mammalian metabolism. This is accompanied by a rapid translational activation of genes encoding mitochondrial, microsomal, and peroxisomal beta-oxidation in the liver, in part under the regulation of peroxisome proliferator-activated receptor-alpha (PPAR-alpha). A failure to express PPAR-alpha results in profound metabolic perturbations in muscle tissue as well as the liver. These changes represent a number of deficits that accompany diabetes, dyslipidemia, and the metabolic syndrome. In this study, the metabolic role of PPAR-alpha has been investigated in heart, skeletal muscle, liver, and adipose tissue of PPAR-alpha null mice at 1 mo of age using metabolomics. To maximize the coverage of the metabolome in these tissues, H-1-NMR spectroscopy, magic angle spinning H-1-NMR spectroscopy, gas chromatography-mass spectrometry, and liquid chromatography-mass spectrometry were used to examine metabolites in aqueous tissue extracts and intact tissue. The data were analyzed by the multivariate approaches of principal components analysis and partial least squares. Across all tissues, there was a profound decrease in glucose and a number of amino acids, including glutamine and alanine, and an increase in lactate, demonstrating that a failure to express PPAR-alpha results in perturbations in glycolysis, the citric acid cycle, and gluconeogenesis. Furthermore, despite PPAR-alpha being weakly expressed in adipose tissue, a profound metabolic perturbation was detected in this tissue.
机译:基于H-1-NMR和质谱的代谢组学研究的PPAR-alpha null突变小鼠定义了与代谢综合征相关的新陈代谢的深刻系统性变化。 Physiol Genomics 27:178-186,2006。首次发布于2006年7月25日; doi:10.1152 /生理基因组学。 00060.2006.-从储存在脂肪细胞中到肝脏的甘油三酸酯的动员是对哺乳动物代谢中禁食状态的重要反应。这伴随着肝脏中编码线粒体,微粒体和过氧化物酶体β-氧化的基因的快速翻译激活,部分是在过氧化物酶体增殖物激活的受体-α(PPAR-α)的调节下。无法表达PPAR-α会导致肌肉组织以及肝脏发生严重的代谢紊乱。这些变化代表糖尿病,血脂异常和代谢综合征伴随的许多缺陷。在这项研究中,已经使用代谢组学研究了在1个月大时PPAR-alpha null小鼠的心脏,骨骼肌,肝脏和脂肪组织中PPAR-alpha的代谢作用。为了最大化代谢物在这些组织中的覆盖范围,H-1NMR光谱,魔角旋转H-1-NMR光谱,气相色谱-质谱和液相色谱-质谱用于检查含水组织提取物中的代谢物和完整的组织。通过主成分分析和偏最小二乘的多元方法分析数据。在所有组织中,葡萄糖和大量氨基酸(包括谷氨酰胺和丙氨酸)大量减少,乳酸含量增加,这表明无法表达PPAR-α会导致糖酵解,柠檬酸循环和糖异生。此外,尽管PPAR-α在脂肪组织中微弱表达,但在该组织中检测到了严重的代谢紊乱。

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