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A method for visualization of “omic” datasets for sphingolipid metabolism to predict potentially interesting differences

机译:一种可视化鞘脂代谢“全基因组”数据集的方法,以预测潜在的有趣差异

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Sphingolipids are structurally diverse and their metabolic pathways highly complex, which makes it difficult to follow all of the subspecies in a biological system, even using "lipidomic" approaches. This report describes a method to use transcriptomic data to visualize and predict potential differences in sphingolipid composition, and it illustrates its use with published data for cancer cell lines and tumors. In addition, several novel sphingolipids that were predicted to differ between MDA-MB-231 and MCF7 cells based on published microarray data for these breast cancer cell lines were confirmed by mass spectrometry. For the data that we were able to find for these comparisons, there was a significant match between the gene expression data and sphingolipid composition (P 0.001 by Fisher's exact test). Upon considering the large number of gene expression datasets produced in recent years, this simple integration of two types of "omic" technologies ("transcriptomics" to direct "sphingolipidomics") might facilitate the discovery of useful relationships between sphingolipid metabolism and disease, such as the identification of new biomarkers.
机译:鞘脂的结构多样,其代谢途径高度复杂,即使使用“脂质组学”方法,也很难追踪生物系统中的所有亚种。该报告描述了一种使用转录组数据可视化并预测鞘脂成分潜在差异的方法,并说明了其与已公开的癌细胞系和肿瘤数据一起使用的方法。另外,通过质谱法证实了基于已公开的这些乳腺癌细胞系的微阵列数据,预计在MDA-MB-231细胞和MCF7细胞之间存在差异的几种新型鞘脂。对于我们能够找到的用于这些比较的数据,基因表达数据与鞘脂成分之间存在显着匹配(Fisher精确检验,P <0.001)。考虑到近年来产生的大量基因表达数据集,两种类型的“组学”技术(“转录组学”指导“鞘脂系统”)的这种简单整合可能有助于发现鞘脂代谢与疾病之间的有用关系,例如新生物标志物的鉴定。

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