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Temporal metabolic profiling of plasma during endotoxemia in humans

机译:时间代谢分析的等离子体内毒素在人类

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摘要

Endotoxemia induced by the administration of low-dose lipopolysaccharide (LPS) to healthy human volunteers is a well-established experimental protocol and has served as a reproducible platform for investigating the responses to systemic inflammation. Because metabolic composition of a tissue or body fluid is uniquely altered by stimuli and provides information about the dominant regulatory mechanisms at various cellular processes, understanding the global metabolic response to systemic inflammation constitutes a major part in this investigation complementing the studies undertaken so far in both clinical and systems biology fields. This article communicates the first proof-of-principle metabonomic analysis, which comprised global biochemical profiles in human plasma samples from healthy subjects given intravenous endotoxin at 2 ng/kg. Concentrations of a total of 366 plasma biochemicals were determined in archived blood samples collected from 15 endotoxin-treated subjects at five time points within 24 h after treatment and compared with control samples collected from four saline-treated subjects. Principal component analysis within this data set determined the sixth hour as a critical time point separating development and recovery phases of the LPS-induced metabolic changes. Consensus clustering of the differential metabolites identified two distinct subsets of metabolites that displayed common coherent profiles with opposing directionality. The first group of metabolites, which were mostly associated with pathways related to lipid metabolism, was upregulated within the first 6 h and downregulated by the 24th hour following LPS administration. The second group of metabolites, in contrast, was first downregulated until the sixth hour, then upregulated. Metabolites in this group were predominantly amino acids or their derivatives. In summary, nontargeted biochemical profiling and unsupervised multivariate analyses highlighted the prominent roles of lipid and protein metabolism in regulating the response to systemic inflammation while also revealing their dynamics in opposite directions.
机译:内毒素诱导的管理低剂量脂多糖(LPS)健康志愿者是一个行之有效的试验协议,并担任可再生的研究平台对全身炎症的反应。组织或体液的代谢成分是唯一被刺激和改变提供了吗占主导地位的管理信息机制在不同的细胞过程,理解全球代谢反应系统性炎症构成的主要部分这次调查补充研究到目前为止进行临床和系统生物学领域。第一原理metabonomic分析,由全球生化资料人血浆样本健康受试者静脉注射内毒素在2 ng /公斤。总共366血浆生化产品确定归档收集血液样本从15 endotoxin-treated五次课程点后24小时内处理和比较从四个控制样本收集saline-treated科目。分析在这个数据集确定六小时作为一个关键时间点分离发展和复苏阶段LPS-induced代谢变化。聚类的差异代谢物确定两个不同的代谢物的子集显示普遍一致的配置文件相反的方向。代谢产物,主要是相关的脂质代谢通路相关,在前6 h和调节表达下调的LPS后24小时管理。相比之下,第一次被下调到六小时,然后调节。主要是氨基酸或其组衍生品。分析和无监督多元分析脂质和强调突出的角色蛋白质代谢调节的响应系统性炎症,同时赋予他们的动力学在相反的方向。

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