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Identification of biomarkers of stent restenosis with serum metabolomic profiling using gas chromatography/mass spectrometry

机译:气相色谱/质谱法通过血清代谢组学鉴定支架再狭窄的生物标志物

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Background: Despite the establishment of guidelines for the secondary prevention of coronary artery diseases, many patients still develop restenosis after stent implantation. Therefore, novel and noninvasive serum biomarkers that can identify restenosis-prone conditions are necessary to improve the follow-up and treatment of patients with coronary artery disease. Of late, considerable attention is being focused on metabolomics, which is the comprehensive analysis of low-molecular-weight metabolites. This study investigated the use of serum metabolomics in the identification of biomarkers of restenosis. Methods and Results: Gas chromatography/mass spectrometry was used to obtain the serum metabolomic profiles of male patients hospitalized for follow-up coronary angiography 6 months after stent implantation; 23 patients presented with major restenotic lesions (≥75% obstruction), 47 with minor restenotic lesions (≤50% obstruction), and 16 with de novo atherosclerotic lesions. Of 83 serum metabolites analyzed, molecules - isobutylamine, sarcosine, homoserine, ribulose, taurine, glutamine, glucose, and tryptophan - in the major restenosis group were significantly different from those in the minor restenosis group. Differences in correlation among these metabolites imply possible alternations in the activated metabolic pathways. Conclusions: This study provides the first line of evidence for the use of serum metabolic profiling in the identification of specific biomarkers of stent restenosis.
机译:背景:尽管建立了二级预防冠状动脉疾病的指南,但许多患者在植入支架后仍出现再狭窄。因此,需要新的,无创的血清生物标志物来识别容易发生再狭窄的疾病,对于改善冠心病患者的随访和治疗是必不可少的。最近,人们对代谢组学进行了相当多的关注,这是对低分子量代谢物的综合分析。这项研究调查了血清代谢组学在再狭窄生物标志物鉴定中的应用。方法与结果:采用气相色谱/质谱法对男性患者进行支架置入6个月后行冠状动脉造影检查后的血清代谢组学特征。 23例患者出现严重的再狭窄病变(≥75%阻塞),47例发生轻微的再狭窄病变(≤50%阻塞)和16例从头发生动脉粥样硬化病变。在主要再狭窄组中,分析的83种血清代谢物中的分子-异丁胺,肌氨酸,高丝氨酸,核糖,牛磺酸,谷氨酰胺,葡萄糖和色氨酸-显着不同于次要再狭窄组。这些代谢物之间相关性的差异意味着激活的代谢途径可能发生交替。结论:这项研究提供了血清代谢谱用于鉴定支架再狭窄的特定生物标志物的第一线证据。

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