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A transgenic zebrafish liver tumor model with inducible Myc expression reveals conserved Myc signatures with mammalian liver tumors

机译:具有可诱导Myc表达的转基因斑马鱼肝肿瘤模型揭示了哺乳动物肝肿瘤的保守Myc信号

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Myc is a pleiotropic transcription factor that is involved in many cellular activities relevant to carcinogenesis, including hepatocarcinogenesis. The zebrafish has been increasingly used to model human diseases and it is particularly valuable in helping to identify common and conserved molecular mechanisms in vertebrates. Here we generated a liver tumor model in transgenic zebrafish by liver-specific expression of mouse Myc using a Tet-On system. Dosage-dependent induction of Myc expression specifically in the liver was observed in our Myc transgenic zebrafish, TO(Myc) , and the elevated Myc expression caused liver hyperplasia, which progressed to hepatocellular adenoma and carcinoma with prolonged induction. Next generation sequencing-based transcriptomic analyses indicated that ribosome proteins were overwhelmingly upregulated in the Myc -induced liver tumors. Cross-species analyses showed that the zebrafish Myc model correlated well with Myc transgenic mouse models for liver cancers. The Myc -induced zebrafish liver tumors also possessed molecular signatures highly similar to human those of hepatocellular carcinoma. Finally, we found that a small Myc target gene set of 16 genes could be used to identify liver tumors due to Myc upregulation. Thus, our zebrafish model demonstrated the conserved role of Myc in promoting hepatocarcinogenesis in all vertebrate species.
机译:Myc是一种多效转录因子,参与许多与癌变有关的细胞活动,包括肝癌的发生。斑马鱼已被越来越多地用于模拟人类疾病,在帮助识别脊椎动物中常见且保守的分子机制方面特别有价值。在这里,我们通过使用Tet-On系统通过小鼠Myc的肝特异性表达在转基因斑马鱼中生成了肝肿瘤模型。在我们的Myc转基因斑马鱼TO(Myc)中观察到剂量依赖性的Myc表达在肝脏中的特异性诱导,并且Myc表达的升高引起肝脏增生,并随着诱导时间的延长发展为肝细胞腺瘤和癌。下一代基于测序的转录组学分析表明,核糖体蛋白在Myc诱导的肝肿瘤中显着上调。跨物种分析表明,斑马鱼Myc模型与Myc转基因小鼠肝癌模型具有很好的相关性。 Myc诱导的斑马鱼肝肿瘤还具有与人类肝细胞癌高度相似的分子特征。最后,我们发现一个由16个基因组成的小型Myc目标基因集可用于鉴定由于Myc上调引起的肝肿瘤。因此,我们的斑马鱼模型证明了Myc在促进所有脊椎动物物种中肝癌发生中的保守作用。

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