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Exploring candidate biomarkers for lung and prostate cancers using gene expression and flux variability analysis

机译:使用基因表达和助焊剂可变性分析探索肺癌和前列腺癌的候选生物标志物

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Genome-scale metabolic models have provided valuable resources for exploring changes in metabolism under normal and cancer conditions. However, metabolism itself is strongly linked to gene expression, so integration of gene expression data into metabolic models might improve the detection of genes involved in the control of tumor progression. Herein, we considered gene expression data as extra constraints to enhance the predictive powers of metabolic models. We reconstructed genome-scale metabolic models for lung and prostate, under normal and cancer conditions to detect the major genes associated with critical subsystems during tumor development. Furthermore, we utilized gene expression data in combination with an information theory-based approach to reconstruct co-expression networks of the human lung and prostate in both cohorts. Our results revealed 19 genes as candidate biomarkers for lung and prostate cancer cells. This study also revealed that the development of a complementary approach (integration of gene expression and metabolic profiles) could lead to proposing novel biomarkers and suggesting renovated cancer treatment strategies which have not been possible to detect using either of the methods alone.
机译:基因组规模的代谢模型提供了有价值的资源,用于探讨正常和癌症条件下新陈代谢的变化。然而,新陈代谢本身与基因表达有密切相关,因此基因表达数据与代谢模型的整合可能改善肿瘤进展控制中涉及的基因的检测。在此,我们将基因表达数据视为额外的约束,以增强代谢模型的预测力。在正常和癌症条件下,在正常和癌症条件下重建基因组级代谢模型,以检测肿瘤发育期间与关键子系统相关的主要基因。此外,我们利用基因表达数据与基于信息理论的方法结合,以重建双群组中的人肺和前列腺的共表达网络。我们的结果揭示了19个基因作为肺癌和前列腺癌细胞的候选生物标志物。本研究还透露,互补方法的发展(基因表达和代谢谱的整合)可能导致提出新的生物标志物并表明未经用途中未经检测的翻译癌症治疗策略。

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