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首页> 外文期刊>Journal of proteome research >Metabolic profiling to identify potential serum biomarkers for gastric ulceration induced by nonsteroid anti-inflammatory drugs
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Metabolic profiling to identify potential serum biomarkers for gastric ulceration induced by nonsteroid anti-inflammatory drugs

机译:代谢谱分析,以鉴定非甾体类抗炎药诱发胃溃疡的潜在血清生物标志物

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摘要

Nonsteroid anti-inflammatory drugs (NSAIDs) are among the most frequently prescribed drugs currently available. The most frequently reported serious side effects associated with NSAIDs are gastric mucosal ulceration and gastric hemorrhage. Presently, these side effects are only detectable by endoscopy, however, and no biomarkers have yet been identified. The ability to identify serum biomarkers would likely improve the safety of NSAID use. In this study we performed capillary electrophoresis-mass spectrometry (CE-MS)-based metabolomic profiling in stomach extract and serum from rats administered NSAIDs. Results showed drug-induced decreases in levels of citrate, cis-aconitate, succinate, 3-hydroxy butanoic acid, o-acetyl carnitine, proline, and hydroxyproline. We consider that these changes are due to NSAID-induced depression of mitochondrial function and activation of collagenase by lesions in the stomach. In addition, four of these changes in metabolite levels in the stomach were significantly correlated with changes in the serum. While further study is needed to clarify the mechanism of change in the level of these biomarkers, limitation of indications, and extrapolation to humans, these new serum biomarker candidates of gastric injury may be useful in the monitoring of NSAID-induced tissue damage.
机译:非甾体类抗炎药(NSAIDs)是目前最常用的处方药。与NSAID相关的最常见的严重副作用是胃粘膜溃疡和胃出血。目前,这些副作用只能通过内窥镜检查来检测,但是,尚未发现任何生物标志物。鉴定血清生物标志物的能力可能会提高NSAID使用的安全性。在这项研究中,我们在接受NSAIDs的大鼠的胃提取物和血清中进行了基于毛细管电泳质谱(CE-MS)的代谢组学分析。结果显示,药物引起的柠檬酸,顺式阿尼酸,琥珀酸,3-羟基丁酸,邻乙酰肉碱,脯氨酸和羟脯氨酸水平降低。我们认为这些变化是由于NSAID引起的线粒体功能降低和胃部病变激活了胶原酶。另外,胃中代谢物水平的这些变化中有四个与血清变化显着相关。尽管需要进一步研究来阐明这些生物标志物水平变化的机制,适应症的局限性以及对人类的外推作用,但这些新的胃损伤血清生物标志物候选物可能在监测NSAID诱导的组织损伤中有用。

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