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Metabolomic Analysis Reveals Distinct Profiles in the Plasma and Urine Associated with IgE Reactions in Childhood Asthma

机译:代谢组学分析揭示了与儿童哮喘IgE反应相关的血浆和尿液中的不同特征

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摘要

Several metabolomics studies have identified altered metabolic pathways that are related to asthma. However, an integrative analysis of the metabolic responses across blood and urine for a comprehensive framework of asthma in early childhood remains lacking. Fifty-four age-matched children with asthma (n = 28) and healthy controls (n = 26) were enrolled. Metabolome analysis of the plasma and urine samples was performed using H-nuclear magnetic resonance (NMR) spectroscopy coupled with partial least-squares discriminant analysis (PLS-DA). Integrated analysis of blood and urine metabolic profiling related to IgE reactions for childhood asthma was investigated. A significantly higher plasma histidine level was found, in parallel with lower urinary 1-methylnicotinamide and trimethylamine N-oxide (TMAO) levels, in children with asthma compared to healthy controls. Compared to children without allergic sensitization, 11 (92%) plasma metabolites and 8 (80%) urinary metabolites were found to be significantly different in children with IgE and food sensitization respectively. There were significant correlations between the plasma 3-hydroxybutyric acid and excreted volumes of the hydroxy acids, which were strongly correlated to plasma leucine and valine levels. Urine N-phenylacetylglycine, a microbial-host co-metabolite, was strongly correlated with total serum and food allergen-specific IgE levels. Plasma pyruvate and urine valine, leucine, and isoleucine degradation metabolisms were significantly associated with allergic sensitization for childhood asthma. In conclusion, blood and urine metabolome reflect different metabolic pathways in allergic reactions. Plasma pyruvate metabolism to acetic acid appears to be associated with serum IgE production, whereas urine branched-chain amino acid metabolism primarily reflects food allergic reactions against allergies.
机译:几项代谢组学研究确定了与哮喘有关的代谢途径改变。但是,仍然缺乏对儿童早期哮喘全面框架中血液和尿液代谢反应的综合分析。入选了54例年龄匹配的哮喘儿童(n = 28)和健康对照者(n = 26)。血浆和尿液样品的代谢组分析是使用H核磁共振(NMR)光谱结合偏最小二乘判别分析(PLS-DA)进行的。研究了与儿童哮喘IgE反应相关的血液和尿液代谢谱的综合分析。与健康对照组相比,哮喘患儿的血浆组氨酸水平明显升高,而尿中的1-甲基烟酰胺和三甲胺N-氧化物(TMAO)水平较低。与没有过敏致敏的儿童相比,IgE和食物致敏儿童的血浆代谢物分别为11(92%)和8(80%)尿代谢物显着不同。血浆3-羟丁酸与羟酸的排泄量之间存在显着相关性,这与血浆亮氨酸和缬氨酸水平密切相关。尿N-苯基乙酰甘氨酸,一种微生物宿主共代谢物,与总血清和食物过敏原特异性IgE水平密切相关。血浆丙酮酸和尿液缬氨酸,亮氨酸和异亮氨酸降解代谢与对儿童哮喘的过敏性致敏作用显着相关。总之,血液和尿液代谢组在过敏反应中反映了不同的代谢途径。血浆丙酮酸代谢成乙酸似乎与血清IgE的产生有关,而尿中的支链氨基酸代谢则主要反映了食物对过敏的过敏反应。

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