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首页> 外文期刊>Journal of Bioinformatics and Computational Biology >Systematic investigation of metabolic reprogramming in different cancers based on tissue-specific metabolic models
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Systematic investigation of metabolic reprogramming in different cancers based on tissue-specific metabolic models

机译:基于组织特异性代谢模型的不同癌症中代谢重编程的系统研究

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Cancer cells have different metabolism in contrast to normal cells. The advancement in omics measurement technology enables the genome-wide characterization of altered cellular processes in cancers, but the metabolic flux landscape of cancer is still far from understood. In this study, we compared the well-reconstructed tissue-specific models of five cancers, including breast, liver, lung, renal, and urothelial cancer, and their corresponding normal cells. There are similar patterns in majority of significantly regulated pathways and enriched pathways in correlated reaction sets. But the differences among cancers are also explicit. The renal cancer demonstrates more dramatic difference with other cancer models, including the smallest number of reactions, flux distribution patterns, and specifically correlated pathways. We also validated the predicted essential genes and revealed the Warburg effect by in silico simulation in renal cancer, which are consistent with the measurements for renal cancer. In conclusion, the tissue-specific metabolic model is more suitable to investigate the cancer metabolism. The similarity and heterogenicity of metabolic reprogramming in different cancers are crucial for understanding the aberrant mechanisms of cancer proliferation, which is fundamental for identifying drug targets and biomarkers.
机译:与正常细胞相比,癌细胞具有不同的代谢。 OMICS测量技术的进步使得能够在癌症中改变细胞过程的全基因组特征,但癌症的代谢助焊剂景观仍远未理解。在这项研究中,我们比较了五种癌症的重建组织特异性模型,包括乳腺癌,肝脏,肺,肾病和尿液癌,以及它们相应的正常细胞。在相关反应集中大多数显着调节的途径和富集的途径存在类似的模式。但癌症之间的差异也是明确的。肾癌与其他癌症模型的差异更大,包括最小的反应,助焊剂分布图案和具体相关的途径。我们还经过验证了预测的必要基因,并通过肾癌中的硅模拟揭示了Warburg效果,这与肾癌的测量一致。总之,组织特异性代谢模型更适合于研究癌症代谢。不同癌症中代谢重编程的相似性和异种性对于了解癌症增殖的异常机制至关重要,这是鉴定药物靶标和生物标志物的基础。

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