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A Translational In Vivo and In Vitro Metabolomic Study Reveals Altered Metabolic Pathways in Red Blood Cells of Type 2 Diabetes

机译:体内和体外代谢组学转化研究揭示了2型糖尿病红细胞中代谢途径的改变

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摘要

Clinical parameters used in type 2 diabetes mellitus (T2D) diagnosis and monitoring such as glycosylated haemoglobin (HbA1c) are often unable to capture important information related to diabetic control and chronic complications. In order to search for additional biomarkers, we performed a pilot study comparing T2D patients with healthy controls matched by age, gender, and weight. By using H-nuclear magnetic resonance (NMR) based metabolomics profiling of red blood cells (RBCs), we found that the metabolic signature of RBCs in T2D subjects differed significantly from non-diabetic controls. Affected metabolites included glutathione, 2,3-bisphophoglycerate, inosinic acid, lactate, 6-phosphogluconate, creatine and adenosine triphosphate (ATP) and several amino acids such as leucine, glycine, alanine, lysine, aspartate, phenylalanine and tyrosine. These results were validated by an independent cohort of T2D and control patients. An analysis of the pathways in which these metabolites were involved showed that energetic and redox metabolism in RBCs were altered in T2D, as well as metabolites transported by RBCs. Taken together, our results revealed that the metabolic profile of RBCs can discriminate healthy controls from T2D patients. Further research is needed to determine whether metabolic fingerprint in RBC could be useful to complement the information obtained from HbA1c and glycemic variability as well as its potential role in the diabetes management.
机译:用于2型糖尿病(T2D)诊断和监测的临床参数,例如糖基化血红蛋白(HbA1c)通常无法捕获与糖尿病控制和慢性并发症有关的重要信息。为了寻找更多的生物标志物,我们进行了一项前瞻性研究,比较了T2D患者和健康对照者的年龄,性别和体重。通过使用基于H核磁共振(NMR)的红细胞(RBC)代谢组学分析,我们发现T2D受试者中RBC的代谢特征与非糖尿病对照显着不同。受影响的代谢产物包括谷胱甘肽,2,3-双磷酸甘油酸酯,肌苷酸,乳酸,6-磷酸葡萄糖酸酯,肌酸和三磷酸腺苷(ATP)以及几种氨基酸,例如亮氨酸,甘氨酸,丙氨酸,赖氨酸,天冬氨酸,苯丙氨酸和酪氨酸。 T2D和对照患者的独立队列验证了这些结果。对涉及这些代谢物的途径的分析表明,在T2D中,RBC中的能量和氧化还原代谢以及RBC转运的代谢物都发生了改变。两者合计,我们的结果表明,RBC的代谢特征可以区分T2D患者的健康对照。需要进行进一步的研究以确定RBC中的代谢指纹是否可用于补充从HbA1c获得的信息和血糖变异性及其在糖尿病管理中的潜在作用。

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