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Portrait of transcriptional responses to ultraviolet and ionizing radiation in human cells

机译:人体细胞对紫外线和电离辐射的转录反应肖像

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摘要

To understand the human response to DNA damage, we used microarrays to measure transcriptional responses of 10 000 genes to ionizing radiation (IR) and ultraviolet radiation (UV). To identify bona fide responses, we used cell lines from 15 individuals and a rigorous statistical method, Significance Analysis of Microarrays (SAM). By exploring how sample number affects SAM, we rendered a portrait of the human damage response with a degree of accuracy unmatched by previous studies. By showing how SAM can be used to estimate the total number of responsive genes, we discovered that 24% of all genes respond to IR and 32% respond to UV, although most responses were less than 2-fold. Many genes were involved in known damage-response pathways for cell cycling and proliferation, apoptosis, DNA repair or the stress response. However, the majority of genes were involved in unexpected pathways, with functions in signal transduction, RNA binding and editing, protein synthesis and degradation, energy metabolism, metabolism of macromolecular precursors, cell structure and adhesion, vesicle transport, or lysosomal metabolism. Although these functions were not previously associated with the damage response in mammals, many were conserved in yeast. These insights reveal new directions for studying the human response to DNA damage.
机译:为了了解人类对DNA损伤的反应,我们使用微阵列来测量10 000个基因对电离辐射(IR)和紫外辐射(UV)的转录反应。为了鉴定真正的反应,我们使用了来自15个个体的细胞系和严格的统计方法,即微阵列的意义分析(SAM)。通过探索样本数量如何影响SAM,我们以人为破坏反应的方式绘制了肖像,其准确性达到了以往研究无法比拟的程度。通过展示如何使用SAM估计响应基因的总数,我们发现所有基因中有24%对IR响应,而32%对UV响应,尽管大多数响应小于2倍。许多基因参与了细胞周期和增殖,凋亡,DNA修复或应激反应的已知损伤反应途径。但是,大多数基因都参与了意想不到的途径,在信号转导,RNA结合和编辑,蛋白质合成和降解,能量代谢,大分子前体的代谢,细胞结构和粘附,囊泡运输或溶酶体代谢中发挥作用。尽管这些功能以前与哺乳动物的损伤反应无关,但许多在酵母中得以保留。这些见解揭示了研究人类对DNA损伤的反应的新方向。

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