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Discovering functional relationships between RNA expression and chemotherapeutic susceptibility using relevance networks

机译:发现RNA表达与 相关网络的化疗敏感性

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摘要

In an effort to find gene regulatory networks and clusters of genes that affect cancer susceptibility to anticancer agents, we joined a database with baseline expression levels of 7,245 genes measured by using microarrays in 60 cancer cell lines, to a database with the amounts of 5,084 anticancer agents needed to inhibit growth of those same cell lines. Comprehensive pair-wise correlations were calculated between gene expression and measures of agent susceptibility. Associations weaker than a threshold strength were removed, leaving networks of highly correlated genes and agents called relevance networks. Hypotheses for potential single-gene determinants of anticancer agent susceptibility were constructed. The effect of random chance in the large number of calculations performed was empirically determined by repeated random permutation testing; only associations stronger than those seen in multiply permuted data were used in clustering. We discuss the advantages of this methodology over alternative approaches, such as phylogenetic-type tree clustering and self-organizing maps.
机译:为了寻找影响癌症对抗癌药敏感性的基因调控网络和基因簇,我们将一个数据库(该数据库具有60245个癌细胞系中的微阵列测量的基线表达水平为7,245个基因)添加到数据库中,该数据库包含5,084个抗癌药物抑制那些相同细胞系生长所需的药物。计算基因表达和药物敏感性之间的综合成对相关性。弱于阈值强度的关联被删除,留下了高度相关的基因和主体的网络,称为关联网络。建立了潜在的抗癌药易感性单基因决定因素的假设。通过重复随机排列检验,经验地确定了随机机会在执行的大量计算中的作用;在聚类中仅使用比在多重排列数据中看到的关联更强的关联。我们讨论了这种方法相对于替代方法(如系统发育型树聚类和自组织图)的优势。

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