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首页> 外文期刊>Journal of the American College of Cardiology >Metabolomic profile of human myocardial ischemia by nuclear magnetic resonance spectroscopy of peripheral blood serum: A translational study based on transient coronary occlusion models
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Metabolomic profile of human myocardial ischemia by nuclear magnetic resonance spectroscopy of peripheral blood serum: A translational study based on transient coronary occlusion models

机译:外周血核磁共振波谱分析人类心肌缺血的代谢组学谱:基于短暂性冠状动脉阻塞模型的转化研究

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Objectives: The aim of this study was to investigate the metabolomic profile of acute myocardial ischemia (MIS) using nuclear magnetic resonance spectroscopy of peripheral blood serum of swine and patients undergoing angioplasty balloon-induced transient coronary occlusion. Background: Biochemical detection of MIS is a major challenge. The validation of novel biosignatures is of utmost importance. Methods: High-resolution nuclear magnetic resonance spectroscopy was used to profile 32 blood serum metabolites obtained (before and after controlled ischemia) from swine (n = 9) and patients (n = 20) undergoing transitory MIS in the setting of planned coronary angioplasty. Additionally, blood serum of control patients (n = 10) was sequentially profiled. Preliminary clinical validation of the developed metabolomic biosignature was undertaken in patients with spontaneous acute chest pain (n = 30). Results: Striking differences were detected in the blood profiles of swine and patients immediately after MIS. MIS induced early increases (10 min) of circulating glucose, lactate, glutamine, glycine, glycerol, phenylalanine, tyrosine, and phosphoethanolamine; decreases in choline-containing compounds and triacylglycerols; and a change in the pattern of total, esterified, and nonesterified fatty acids. Creatine increased 2 h after ischemia. Using multivariate analyses, a biosignature was developed that accurately detected patients with MIS both in the setting of angioplasty-related MIS (area under the curve 0.94) and in patients with acute chest pain (negative predictive value 95%). Conclusions: This study reports, to the authors' knowledge, the first metabolic biosignature of acute MIS developed under highly controlled coronary flow restriction. Metabolic profiling of blood plasma appears to be a promising approach for the early detection of MIS in patients.
机译:目的:本研究的目的是使用猪和接受血管成形术球囊引起的短暂性冠状动脉闭塞的患者外周血核磁共振波谱研究急性心肌缺血(MIS)的代谢组学特征。背景:MIS的生化检测是一项重大挑战。新型生物特征的验证至关重要。方法:采用高分辨率核磁共振波谱法,对在计划性冠状动脉成形术中从猪(n = 9)和经历短暂性MIS的患者(n = 20)中获得的32种血清代谢产物(受控缺血前后)进行了分析。另外,顺序分析了对照患者(n = 10)的血清。对患有自发性急性胸痛(n = 30)的患者进行了代谢组学生物特征的初步临床验证。结果:MIS后立即在猪和患者的血液中发现惊人的差异。 MIS引起循环葡萄糖,乳酸,谷氨酰胺,甘氨酸,甘油,苯丙氨酸,酪氨酸和磷酸乙醇胺的早期增加(10分钟);减少胆碱化合物和三酰基甘油;以及总,酯化和非酯化脂肪酸的模式发生变化。缺血2小时后肌酸增加。使用多变量分析,开发了一种生物特征,可以在血管成形术相关的MIS(曲线下面积0.94)和急性胸痛(阴性预测值95%)患者中准确检测出MIS患者。结论:据作者所知,该研究报道了在高度受控的冠状动脉血流限制下发展的急性MIS的首个代谢生物特征。血浆的代谢谱分析似乎是早期检测患者MIS的有前途的方法。

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