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Prediction of a gene regulatory network linked to prostate cancer from gene expression, microRNA and clinical data

机译:从基因表达,microRNa和临床数据预测与前列腺癌相关的基因调控网络

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摘要

Motivation: Cancer is a complex disease, triggered by mutations in multiple genes and pathways. There is a growing interest in the application of systems biology approaches to analyze various types of cancer-related data to understand the overwhelming complexity of changes induced by the disease.Results: We reconstructed a regulatory module network using gene expression, microRNA expression and a clinical parameter, all measured in lymphoblastoid cell lines derived from patients having aggressive or non-aggressive forms of prostate cancer. Our analysis identified several modules enriched in cell cycle-related genes as well as novel functional categories that might be linked to prostate cancer. Almost one-third of the regulators predicted to control the expression levels of the modules are microRNAs. Several of them have already been characterized as causal in various diseases, including cancer. We also predicted novel microRNAs that have never been associated to this type of tumor. Furthermore, the condition-dependent expression of several modules could be linked to the value of a clinical parameter characterizing the aggressiveness of the prostate cancer. Taken together, our results help to shed light on the consequences of aggressive and non-aggressive forms of prostate cancer.
机译:动机:癌症是一种复杂的疾病,由多种基因和途径的突变触发。系统生物学方法用于分析各种类型的与癌症相关的数据以了解由疾病引起的变化的复杂性的兴趣日益浓厚。结果:我们使用基因表达,microRNA表达和临床重建了一个调控模块网络。参数,所有参数均来自患有侵袭性或非侵袭性前列腺癌患者的淋巴母细胞系。我们的分析确定了几个富含细胞周期相关基因的模块,以及可能与前列腺癌相关的新功能类别。预计将控制模块表达水平的调节子中,几乎有三分之一是微RNA。其中一些已经被归类为包括癌症在内的各种疾病的病因。我们还预测了从未与这种类型的肿瘤相关的新型microRNA。此外,几个模块的条件依赖性表达可以与表征前列腺癌的侵袭性的临床参数的值联系起来。综上所述,我们的研究结果有助于阐明侵略性和非侵略性前列腺癌的后果。

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