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Application of comparative functional genomics to identify best-fit mouse models to study human cancer

机译:比较功能基因组学在识别最适合研究人类癌症的小鼠模型中的应用

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摘要

Genetically modified mice have been extensively used for analyzing the molecular events that occur during tumor development. In many, if not all, cases, however, it is uncertain to what extent the mouse models reproduce features observed in the corresponding human conditions(1-3). This is due largely to lack of precise methods for direct and comprehensive comparison at the molecular level of the mouse and human tumors. Here we use global gene expression patterns of 68 hepatocellular carcinomas (HCCs) from seven different mouse models and 91 human HCCs from predefined subclasses(4) to obtain direct comparison of the molecular features of mouse and human HCCs. Gene expression patterns in HCCs from Myc, E2f1 and Myc E2f1 transgenic mice were most similar to those of the better survival group of human HCCs, whereas the expression patterns in HCCs from Myc Tgfa transgenic mice and in diethylnitrosamine-induced mouse HCCs were most similar to those of the poorer survival group of human HCCs. Gene expression patterns in HCCs from Acox1(-/-) mice and in ciprofibrate-induced HCCs were least similar to those observed in human HCCs. We conclude that our approach can effectively identify appropriate mouse models to study human cancers.
机译:转基因小鼠已被广泛用于分析肿瘤发展过程中发生的分子事件。然而,在很多情况下(即使不是全部),也无法确定小鼠模型在多大程度上可重现在相应人类条件下观察到的特征(1-3)。这主要是由于缺乏用于在小鼠和人类肿瘤的分子水平上进行直接和全面比较的精确方法。在这里,我们使用来自七个不同小鼠模型的68个肝细胞癌(HCC)和来自预定义亚类的4个人类HCC的全局基因表达模式(4),来直接比较小鼠和人类HCC的分子特征。 Myc,E2f1和Myc E2f1转基因小鼠的HCC中的基因表达模式与存活率更高的人类HCC组最相似,而Myc Tgfa转基因小鼠的HCC和二乙基亚硝胺诱导的小鼠HCC中的基因表达模式最相似。那些人类肝癌生存率较低的人群。来自Acox1(-/-)小鼠和环丙酸盐诱导的HCC中HCC的基因表达模式与人类HCC中观察到的基因表达模式最不相似。我们得出结论,我们的方法可以有效地识别合适的小鼠模型来研究人类癌症。

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