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首页> 外文期刊>Journal of molecular cell biology >Gene dysregulation analysis builds a mechanistic signature for prognosis and therapeutic benefit in colorectal cancer
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Gene dysregulation analysis builds a mechanistic signature for prognosis and therapeutic benefit in colorectal cancer

机译:基因失调分析建立了成直肠癌预后和治疗益处的机制签名

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The implementation of cancer precision medicine requires biomarkers or signatures for predicting prognosis and therapeutic benefits. Most of current efforts in this field are paying much more attention to predictive accuracy than to molecular mechanistic interpretability. Mechanism-driven strategy has recently emerged, aiming to build signatures with both predictive power and explanatory power. Driven by this strategy, we developed a robust gene dysregulation analysis framework with machine learning algorithms, which is capable of exploring gene dysregulations underlying carcinogenesis from high-dimensional data with cooperativity and synergy between regulators and several other transcriptional regulation rules taken into consideration. We then applied the framework to a colorectal cancer (CRC) cohort from The Cancer Genome Atlas. The identified CRC-related dysregulations significantly covered known carcinogenic processes and exhibited good prognostic effect. By choosing dysregulations with greedy strategy, we built a four-dysregulation (4-DysReg) signature, which has the capability of predicting prognosis and adjuvant chemotherapy benefit. 4-DysReg has the potential to explain carcinogenesis in terms of dysfunctional transcriptional regulation. These results demonstrate that our gene dysregulation analysis framework could be used to develop predictive signature with mechanistic interpretability for cancer precision medicine, and furthermore, elucidate the mechanisms of carcinogenesis.
机译:癌症精密药物的实施需要用于预测预后和治疗益处的生物标志物或签名。该领域的最新努力的努力更加注重预测准确性,而不是分子机械解释性。最近出现了机制驱动的策略,旨在构建具有预测力和解释性的签名。通过这种策略驱动,我们开发了一种具有机器学习算法的强大基因失调分析框架,其能够从高维数据探索基因失调癌症,以及调节因子之间的合作和协同作用以及考虑的其他几个转录规则。然后,我们将框架应用于从癌症基因组地图集的结肠直肠癌(CRC)队列。鉴定的CRC相关的呼吸缺陷显着涵盖了已知的致癌方法,并表现出良好的预后效果。通过使用贪婪的策略选择疑难解失用,我们构建了一个四个失去的(4-Dysreg)签名,具有预测预后和佐剂化疗的能力。 4-Dysreg有可能在功能障碍转录调节方面解释致癌作用。这些结果表明,我们的基因失调分析框架可用于开发具有癌症精密药物的机械解释性的预测性签名,此外,阐明致癌物的机制。

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