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Aptamer-based search for correlates of plasma and serum water T 2 : implications for early metabolic dysregulation and metabolic syndrome

机译:基于适体的血浆和血清水T 2相关性搜索:对早期代谢失调和代谢综合征的影响

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Background Metabolic syndrome is a cluster of abnormalities that increases the risk for type 2 diabetes and atherosclerosis. Plasma and serum water T2 from benchtop nuclear magnetic resonance relaxometry are early, global and practical biomarkers for metabolic syndrome and its underlying abnormalities. In a prior study, water T2 was analyzed against ~?130 strategically selected proteins and metabolites to identify associations with insulin resistance, inflammation and dyslipidemia. In the current study, the analysis was broadened ten-fold using a modified aptamer (SOMAmer) library, enabling an unbiased search for new proteins correlated with water T2 and thus, metabolic health. Methods Water T2 measurements were recorded using fasting plasma and serum from non-diabetic human subjects. In parallel, plasma samples were analyzed using a SOMAscan assay that employed modified DNA aptamers to determine the relative concentrations of 1310 proteins. A multi-step statistical analysis was performed to identify the biomarkers most predictive of water T2. The steps included Spearman rank correlation, followed by principal components analysis with variable clustering, random forests for biomarker selection, and regression trees for biomarker ranking. Results The multi-step analysis unveiled five new proteins most predictive of water T2: hepatocyte growth factor, receptor tyrosine kinase FLT3, bone sialoprotein 2, glucokinase regulatory protein and endothelial cell-specific molecule 1. Three of the five strongest predictors of water T2 have been previously implicated in cardiometabolic diseases. Hepatocyte growth factor has been associated with incident type 2 diabetes, and endothelial cell specific molecule 1, with atherosclerosis in subjects with diabetes. Glucokinase regulatory protein plays a critical role in hepatic glucose uptake and metabolism and is a drug target for type 2 diabetes. By contrast, receptor tyrosine kinase FLT3 and bone sialoprotein 2 have not been previously associated with metabolic conditions. In addition to the five most predictive biomarkers, the analysis unveiled other strong correlates of water T2 that would not have been identified in a hypothesis-driven biomarker search. Conclusions The identification of new proteins associated with water T2 demonstrates the value of this approach to biomarker discovery. It provides new insights into the metabolic significance of water T2 and the pathophysiology of metabolic syndrome.
机译:背景代谢综合征是一类异常现象,会增加2型糖尿病和动脉粥样硬化的风险。台式核磁共振弛豫法测定的血浆和血清水T2是代谢综合征及其潜在异常的早期,全局和实用的生物标志物。在先前的研究中,对水T2进行了约130种战略选择的蛋白质和代谢物分析,以鉴定与胰岛素抵抗,炎症和血脂异常的相关性。在当前研究中,使用改良的适体(SOMAmer)文库将分析范围扩大了十倍,从而能够无偏搜索与水T2相关的新蛋白质,从而实现代谢健康。方法使用非糖尿病人受试者的空腹血浆和血清记录水T2的测量值。平行地,使用SOMAscan测定法分析血浆样品,该测定法采用修饰的DNA适体来确定1310蛋白的相对浓度。进行了多步统计分析,以确定最能预测水T2的生物标志物。这些步骤包括Spearman等级相关性,然后进行具有可变聚类的主成分分析,用于生物标记选择的随机森林以及用于生物标记排名的回归树。结果多步骤分析揭示了五个最能预测水T2的新蛋白:肝细胞生长因子,受体酪氨酸激酶FLT3,骨唾液蛋白2,葡萄糖激酶调节蛋白和内皮细胞特异性分子1。五个最强的预测水T2的蛋白质中有三个以前与心脏代谢疾病有关。肝细胞生长因子已与2型糖尿病相关,而内皮细胞特异性分子1与糖尿病患者的动脉粥样硬化相关。葡萄糖激酶调节蛋白在肝葡萄糖摄取和代谢中起关键作用,并且是2型糖尿病的药物靶标。相比之下,受体酪氨酸激酶FLT3和骨唾液蛋白2以前与代谢状况无关。除了五个最具预测性的生物标记物之外,该分析还揭示了水T2的其他强相关性,这些相关性在假设驱动的生物标记物搜索中无法确定。结论对与水T2相关的新蛋白质的鉴定证明了该方法对生物标记物发现的价值。它为水T2的代谢意义和代谢综合征的病理生理学提供了新的见解。

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