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首页> 外文期刊>BMC Genomics >Novel functional view of the crocidolite asbestos-treated A549 human lung epithelial transcriptome reveals an intricate network of pathways with opposing functions
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Novel functional view of the crocidolite asbestos-treated A549 human lung epithelial transcriptome reveals an intricate network of pathways with opposing functions

机译:青石棉石棉处理过的A549人肺上皮转录组的新颖功能性观点揭示了功能相反的复杂通路网络

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Background Although exposure to asbestos is now regulated, patients continue to be diagnosed with mesothelioma, asbestosis, fibrosis and lung carcinoma because of the long latent period between exposure and clinical disease. Asbestosis is observed in approximately 200,000 patients annually and asbestos-related deaths are estimated at 4,000 annually [ 1 ]. Although advances have been made using single gene/gene product or pathway studies, the complexity of the response to asbestos and the many unanswered questions suggested the need for a systems biology approach. The objective of this study was to generate a comprehensive view of the transcriptional changes induced by crocidolite asbestos in A549 human lung epithelial cells. Results A statistically robust, comprehensive data set documenting the crocidolite-induced changes in the A549 transcriptome was collected. A systems biology approach involving global observations from gene ontological analyses coupled with functional network analyses was used to explore the effects of crocidolite in the context of known molecular interactions. The analyses uniquely document a transcriptome with function-based networks in cell death, cancer, cell cycle, cellular growth, proliferation, and gene expression. These functional modules show signs of a complex interplay between signaling pathways consisting of both novel and previously described asbestos-related genes/gene products. These networks allowed for the identification of novel, putative crocidolite-related genes, leading to several new hypotheses regarding genes that are important for the asbestos response. The global analysis revealed a transcriptome that bears signatures of both apoptosis/cell death and cell survival/proliferation. Conclusion Our analyses demonstrate the power of combining a statistically robust, comprehensive dataset and a functional network genomics approach to 1) identify and explore relationships between genes of known importance 2) identify novel candidate genes, and 3) observe the complex interplay between genes/gene products that function in seemingly different processes. This study represents the first function-based global approach toward understanding the response of human lung epithelial cells to the carcinogen crocidolite. Importantly, our investigation paints a much broader landscape for the crocidolite response than was previously appreciated and reveals novel paths to study. Our graphical representations of the function-based global network will be a valuable resource to model new research findings.
机译:背景技术尽管现在对石棉的接触进行了管制,但由于接触和临床疾病之间的潜伏期长,因此继续诊断出患有间皮瘤,石棉沉着症,纤维化和肺癌。每年约有200,000名患者观察到石棉病,估计每年与石棉有关的死亡为4,000 [1]。尽管使用单基因/基因产物或途径研究取得了进展,但是对石棉的反应的复杂性和许多未解决的问题表明需要系统生物学方法。这项研究的目的是全面了解青石棉石棉在A549人肺上皮细胞中诱导的转录变化。结果收集了统计可靠的综合数据集,该数据集记录了青石棉石引起的A549转录组的变化。一种系统生物学方法,涉及从基因本体论分析中进行的全局观察以及功能网络分析,用于探讨青石棉在已知分子相互作用情况下的作用。这些分析独特地记录了一个转录组,该转录组在细胞死亡,癌症,细胞周期,细胞生长,增殖和基因表达中具有基于功能的网络。这些功能模块显示出信号通路之间复杂相互作用的迹象,该信号通路既包括新的又涉及先前描述的石棉相关基因/基因产物。这些网络允许鉴定新颖的,与青石棉有关的基因,从而导致有关对石棉反应重要的基因的若干新假设。整体分析揭示了一个转录组,其具有凋亡/细胞死亡和细胞存活/增殖的特征。结论我们的分析表明,结合强大的统计数据集和功能网络基因组学方法,可以实现1)识别和探索已知重要性基因之间的关系2)识别新的候选基因,以及3)观察基因/基因之间复杂的相互作用在看似不同的过程中起作用的产品。这项研究代表了了解人类肺上皮细胞对致癌物质青石棉的反应的第一个基于功能的全局方法。重要的是,我们的调查为青石棉反应画了比以前更广阔的视野,并揭示了新颖的研究途径。我们基于功能的全球网络的图形表示将成为建模新研究结果的宝贵资源。

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