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首页> 外文期刊>Diabetes, metabolic syndrome and obesity: targets and therapy >Detection of Secondary Metabolites as Biomarkers for the Early Diagnosis and Prevention of Type 2 Diabetes
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Detection of Secondary Metabolites as Biomarkers for the Early Diagnosis and Prevention of Type 2 Diabetes

机译:检测次级代谢产物作为生物标志物,用于早期诊断和预防2型糖尿病

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Background: Type 2 diabetes, or T2D, is a metabolic disease that results in insulin resistance. In the present study, we hypothesize that metabolomic analysis in blood samples of T2D patients sharing the same ethnic background can recover new metabolic biomarkers and pathways that elucidate early diagnosis and predict the incidence of T2D. Methods: The study included 34 T2D patients and 33 healthy volunteers recruited between the years 2012 and 2013; the secondary metabolites were extracted from blood samples and analyzed using HPLC. Results: Principal coordinate analysis and hierarchical clustering patterns for the uncharacterized negatively and positively charged metabolites indicated that samples from healthy individuals and T2D patients were largely separated with only a few exceptions. The inspection of the top 10% secondary metabolites indicated an increase in fucose, tryptophan and choline levels in the T2D patients, while there was a reduction in carnitine, homoserine, allothreonine, serine and betaine as compared to healthy individuals. These metabolites participate mainly in three cross-talking pathways, namely “glucagon signaling”, “glycine, serine and threonine” and “bile secretion”. Reduced level of carnitine in T2D patients is known to participate in the impaired insulin-stimulated glucose utilization, while reduced betaine level in T2D patients is known as a common feature of this metabolic syndrome and can result in the reduced glycine production and the occurrence of insulin resistance. However, reduced levels of serine, homoserine and allothrionine, substrates for glycine production, indicate the depletion of glycine, thus possibly impair insulin sensitivity in T2D patients of the present study. Conclusion: We introduce serine, homoserine and allothrionine as new potential biomarkers of T2D.
机译:背景:2型糖尿病或T2D,是一种导致胰岛素抗性的代谢疾病。在本研究中,我们假设分享同一种族背景的T2D患者的血液样本中的代谢组分可以恢复阐明早期诊断和预测T2D发病率的新代谢生物标志物和途径。方法:该研究包括34名T2D患者,2012年和2013年之间招募了33名健康志愿者;次级代谢物从血液样品中提取并使用HPLC分析。结果:针对无特征化负性和带正电荷的代谢物的主坐标分析和分层聚类模式表明,来自健康个体和T2D患者的样本在很大程度上分开了一些例外。前10%次级代谢产物的检查表明,与健康个体相比,肉桂糖,色氨酸和胆碱水平的增加,而肉毒碱,肉碱,甲状腺素,丝氨酸和甜菜碱等含量增加。这些代谢物主要参与三个交叉谈话途径,即“胰高血糖素信号”,“甘氨酸,丝氨酸和苏氨酸”和“胆汁分泌”。已知T2D患者肉碱水平降低参与胰岛素刺激的葡萄糖利用损害,而T2D患者的降低的甜菜碱水平被称为该代谢综合征的常见特征,可导致甘氨酸产生降低和胰岛素的发生。抵抗性。然而,降低了丝氨酸,甲络石和含有甘氨酸碱的底物的水平,表明甘氨酸的耗竭,因此可能在本研究的T2D患者中患有胰岛素敏感性。结论:我们将丝氨酸,甲丝和含有T2D的新潜在生物标志物介绍。

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