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Proteomic and Metabolomic Analyses Reveal Contrasting Anti-Inflammatory Effects of an Extract of Mucor Racemosus Secondary Metabolites Compared to Dexamethasone

机译:蛋白质组学和代谢组学分析显示与地塞米松相比Mucor Racemosus次生代谢产物提取物具有相反的抗炎作用

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摘要

Classical drug assays are often confined to single molecules and targeting single pathways. However, it is also desirable to investigate the effects of complex mixtures on complex systems such as living cells including the natural multitude of signalling pathways. Evidence based on herbal medicine has motivated us to investigate potential beneficial health effects of Mucor racemosus (M rac) extracts. Secondary metabolites of M rac were collected using a good-manufacturing process (GMP) approved production line and a validated manufacturing process, in order to obtain a stable product termed SyCircue (National Drug Code USA: 10424–102). Toxicological studies confirmed that this product does not contain mycotoxins and is non-genotoxic. Potential effects on inflammatory processes were investigated by treating stimulated cells with M rac extracts and the effects were compared to the standard anti-inflammatory drug dexamethasone on the levels of the proteome and metabolome. Using 2D-PAGE, slight anti-inflammatory effects were observed in primary white blood mononuclear cells, which were more pronounced in primary human umbilical vein endothelial cells (HUVECs). Proteome profiling based on nLC-MS/MS analysis of tryptic digests revealed inhibitory effects of M rac extracts on pro-inflammatory cytoplasmic mediators and secreted cytokines and chemokines in these endothelial cells. This finding was confirmed using targeted proteomics, here treatment of stimulated cells with M rac extracts down-regulated the secretion of IL-6, IL-8, CXCL5 and GROA significantly. Finally, the modulating effects of M rac on HUVECs were also confirmed on the level of the metabolome. Several metabolites displayed significant concentration changes upon treatment of inflammatory activated HUVECs with the M rac extract, including spermine and lysophosphatidylcholine acyl C18:0 and sphingomyelin C26:1, while the bulk of measured metabolites remained unaffected. Interestingly, the effects of M rac treatment on lipids were orthogonal to the effect of dexamethasone underlining differences in the overall mode of action.
机译:经典药物测定法通常仅限于单个分子并靶向单个途径。但是,还希望研究复杂混合物对复杂系统(例如活细胞)的影响,其中包括天然的多种信号通路。基于草药的证据促使我们研究了总状木提取物的潜在有益健康作用。为了获得称为SyCircue的稳定产品(美国国家药品代码:10424–102),使用经过良好生产工艺(GMP)批准的生产线和经过验证的生产工艺来收集M rac的次级代谢产物。毒理学研究证实,该产品不含霉菌毒素,无遗传毒性。通过用M rac提取物处理刺激的细胞来研究对炎症过程的潜在影响,并将其与蛋白质组和代谢组水平的标准抗炎药地塞米松进行比较。使用2D-PAGE,在原代白血单个核细胞中观察到了轻微的抗炎作用,在原代人脐静脉内皮细胞(HUVEC)中更为明显。基于胰蛋白酶消化物的nLC-MS / MS分析进行的蛋白质组分析显示,M rac提取物对这些内皮细胞中促炎性细胞质介质以及分泌的细胞因子和趋化因子具有抑制作用。使用靶向蛋白质组学证实了这一发现,此处用M rac提取物处理刺激的细胞可显着下调IL-6,IL-8,CXCL5和GROA的分泌。最后,还证实了M rac对HUVEC的调节作用。用M rac提取物治疗炎症激活的HUVEC时,几种代谢物显示出明显的浓度变化,包括精胺和溶血磷脂酰胆碱酰基C18:0和鞘磷脂C26:1,而大部分测得的代谢物仍不受影响。有趣的是,M rac治疗对脂质的作用与地塞米松的作用正交,这强调了整体作用方式的差异。

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