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Biological and functional analysis of statistically significant pathways deregulated in colon cancer by using gene expression profiles

机译:使用基因表达谱对结肠癌中失控的统计学上重要途径的生物学和功能分析

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摘要

Gene expression profiling offers a great opportunity for studying multi-factor diseases and for understanding the key role of genes in mechanisms which drive a normal cell to a cancer state. Single gene analysis is insufficient to describe the complex perturbations responsible for cancer onset, progression and invasion. A deeper understanding of the mechanisms of tumorigenesis can be reached focusing on deregulation of gene sets or pathways rather than on individual genes. We apply two known and statistically well founded methods for finding pathways and biological processes deregulated in pathological conditions by analyzing gene expression profiles. In particular, we measure the amount of deregulation and assess the statistical significance of predefined pathways belonging to a curated collection (Molecular Signature Database) in a colon cancer data set. We find that pathways strongly involved in different tumors are strictly connected with colon cancer. Moreover, our experimental results show that the study of complex diseases through pathway analysis is able to highlight genes weakly connected to the phenotype which may be difficult to detect by using classical univariate statistics. Our study shows the importance of using gene sets rather than single genes for understanding the main biological processes and pathways involved in colorectal cancer. Our analysis evidences that many of the genes involved in these pathways are strongly associated to colorectal tumorigenesis. In this new perspective, the focus shifts from finding differentially expressed genes to identifying biological processes, cellular functions and pathways perturbed in the phenotypic conditions by analyzing genes co-expressed in a given pathway as a whole, taking into account the possible interactions among them and, more importantly, the correlation of their expression with the phenotypical conditions.
机译:基因表达谱分析为研究多因素疾病和理解基因在将正常细胞驱动至癌症状态的机制中的关键作用提供了巨大的机会。单基因分析不足以描述导致癌症发作,进展和侵袭的复杂扰动。对肿瘤发生机理的更深入了解可以集中在基因集或途径的失调而不是单个基因上。我们通过分析基因表达谱,应用两种已知且统计学上公认的方法来寻找病理条件下失控的途径和生物学过程。特别是,我们测量了放松管制的数量,并评估了结肠癌数据集中属于策展性集合的预定义途径(分子签名数据库)的统计意义。我们发现强烈参与不同肿瘤的通路与结肠癌严格相关。此外,我们的实验结果表明,通过途径分析对复杂疾病进行研究能够突出显示与表型相关性较弱的基因,而这些基因可能很难通过经典单变量统计法进行检测。我们的研究表明,使用基因组而不是单个基因来了解结直肠癌的主要生物学过程和途径非常重要。我们的分析证明,这些途径中涉及的许多基因与结直肠肿瘤发生密切相关。在这个新的视角下,研究重点从寻找差异表达的基因转向通过分析共同在给定途径中共表达的基因,并考虑到它们之间可能存在的相互作用,来识别在表型条件下受到干扰的生物学过程,细胞功能和途径。更重要的是,它们的表达与表型条件的相关性。

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