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Optimized Method for Untargeted Metabolomics Analysis of MDA-MB-231 Breast Cancer Cells

机译:MDA-MB-231乳腺癌细胞非靶向代谢组学分析的优化方法

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摘要

Cancer cells often have dysregulated metabolism, which is largely characterized by the Warburg effect—an increase in glycolytic activity at the expense of oxidative phosphorylation—and increased glutamine utilization. Modern metabolomics tools offer an efficient means to investigate metabolism in cancer cells. Currently, a number of protocols have been described for harvesting adherent cells for metabolomics analysis, but the techniques vary greatly and they lack specificity to particular cancer cell lines with diverse metabolic and structural features. Here we present an optimized method for untargeted metabolomics characterization of MDA-MB-231 triple negative breast cancer cells, which are commonly used to study metastatic breast cancer. We found that an approach that extracted all metabolites in a single step within the culture dish optimally detected both polar and non-polar metabolite classes with higher relative abundance than methods that involved removal of cells from the dish. We show that this method is highly suited to diverse applications, including the characterization of central metabolic flux by stable isotope labelling and differential analysis of cells subjected to specific pharmacological interventions.
机译:癌细胞通常代谢失调,主要表现为Warburg效应-糖酵解活性的增加(以氧化磷酸化为代价)和谷氨酰胺利用的增加。现代代谢组学工具提供了研究癌细胞中新陈代谢的有效手段。当前,已经描述了用于收集用于代谢组学分析的贴壁细胞的许多方案,但是技术差异很大,并且它们对具有多种代谢和结构特征的特定癌细胞系缺乏特异性。在这里,我们为MDA-MB-231三阴性乳腺癌细胞的非靶向代谢组学表征提供了一种优化方法,该细胞通常用于研究转移性乳腺癌。我们发现,与在培养皿中去除细胞的方法相比,在培养皿中一步提取所有代谢物的方法可最佳地检测极性和非极性代谢物类别,且相对丰度更高。我们表明该方法非常适合各种应用,包括通过稳定的同位素标记和对经过特定药理学干预的细胞进行差异分析来表征中心代谢通量。

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