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Microarray Data Mining for Potential Selenium Targets in Chemoprevention of Prostate Cancer

机译:前列腺癌化学预防中潜在硒靶点的微阵列数据挖掘

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A previous clinical trial showed that selenium supplementation significantly reduced the incidence of prostate cancer. We report here a bioinforniatics approach to gain new insights into selenium molecular targets that might be relevant to prostate cancer chemoprevention. Materials and Methods: We first performed data mining analysis to identify genes which are consistently dysregulated in prostate cancer using published datasets from gene expression profiling of clinical prostate specimens. We then devised a method to systematically analyze three selenium microarray datasets from the LNCaP human prostate cancer cells, and to match the analysis to the cohort of genes implicated in prostate carcinogenesis. Moreover, we compared the selenium datasets with two datasets obtained from expression profiling of androgen-stimulated LNCaP cells. Results: We found that selenium reverses the expression of genes implicated in prostate carcinogenesis. In addition, we found that selenium could counteract the effect of androgen on the expression of a subset obtained from androgen-regulated genes. Conclusions: The above information provides us with a treasure of new clues to investigate the mechanism of selenium chemoprevention of prostate cancer. Furthermore, these selenium target genes could also serve as biomarkers in future clinical trials to gauge the efficacy of selenium intervention.
机译:先前的一项临床试验表明,补充硒可显着降低前列腺癌的发病率。我们在这里报告一种生物信息学方法,以获取对可能与前列腺癌化学预防有关的硒分子靶标的新见解。材料和方法:我们首先进行了数据挖掘分析,以使用来自临床前列腺标本的基因表达谱的已公开数据集来鉴定在前列腺癌中始终失调的基因。然后,我们设计了一种方法,可以从LNCaP人前列腺癌细胞中系统分析三个硒微阵列数据集,并使该分析与涉及前列腺癌发生的基因队列相匹配。此外,我们将硒数据集与从雄激素刺激的LNCaP细胞表达谱获得的两个数据集进行了比较。结果:我们发现硒逆转了与前列腺癌发生有关的基因的表达。此外,我们发现硒可以抵消雄激素对从雄激素调节基因获得的子集表达的影响。结论:以上信息为我们提供了一些新的线索,可用于研究硒化学预防前列腺癌的机制。此外,这些硒靶基因还可以在未来的临床试验中用作生物标记物,以评估硒干预的功效。

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