May Merav, Elnatan M Bitensky, Elisheva E Heilbrun, Tamar Hacohen, Ayala Kirshenbaum, Hadar Golan-Berman, Yuval Cohen, Sheera Adar
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引用次数: 0
摘要
大块 DNA 损伤会阻碍转录,损害基因组的完整性和功能。细胞对这些损伤的反应包括全面的转录关闭。但是,活跃的转录对于转录耦合修复和损伤反应基因的诱导仍然是必要的。为了揭示普遍的大量 DNA 损伤反应的共同特征,并确定在损伤情况下仍能表达的与反应相关的转录本,我们进行了一项系统的 RNA-seq 研究,比较了对三种独立的损伤诱导剂的转录反应:紫外线、化疗药物顺铂和香烟烟雾中的一种成分苯并[a]芘。损伤后基因表达的减少与较高的损伤率、较长的基因长度和较低的 GC 含量有关。我们发现了在所有三种损伤处理后表达相对较高的基因,包括潜在的新型损伤反应转录因子 NR4A2。上调基因表现出较高的外显子含量,这与优先修复有关,可使损伤快速消除和转录恢复。对 BPDE 的反应减弱突出表明,并非所有大体积损伤都会引起相同的反应。这些发现表明,基因结构是人类基因组转录反应的主要决定因素。
Gene architecture is a determinant of the transcriptional response to bulky DNA damages.
Bulky DNA damages block transcription and compromise genome integrity and function. The cellular response to these damages includes global transcription shutdown. Still, active transcription is necessary for transcription-coupled repair and for induction of damage-response genes. To uncover common features of a general bulky DNA damage response, and to identify response-related transcripts that are expressed despite damage, we performed a systematic RNA-seq study comparing the transcriptional response to three independent damage-inducing agents: UV, the chemotherapy cisplatin, and benzo[a]pyrene, a component of cigarette smoke. Reduction in gene expression after damage was associated with higher damage rates, longer gene length, and low GC content. We identified genes with relatively higher expression after all three damage treatments, including NR4A2, a potential novel damage-response transcription factor. Up-regulated genes exhibit higher exon content that is associated with preferential repair, which could enable rapid damage removal and transcription restoration. The attenuated response to BPDE highlights that not all bulky damages elicit the same response. These findings frame gene architecture as a major determinant of the transcriptional response that is hardwired into the human genome.
期刊介绍:
Life Science Alliance is a global, open-access, editorially independent, and peer-reviewed journal launched by an alliance of EMBO Press, Rockefeller University Press, and Cold Spring Harbor Laboratory Press. Life Science Alliance is committed to rapid, fair, and transparent publication of valuable research from across all areas in the life sciences.