Simona Cantarella, Marco Vezzoli, Davide Carnevali, Marco Morselli, Nathan R Zemke, Barbara Montanini, Coralie F Daussy, Harald Wodrich, Martin Teichmann, Matteo Pellegrini, Arnold J Berk, Giorgio Dieci, Roberto Ferrari
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引用次数: 0
摘要
Alu 反转座子是人类基因组中最大的移动 DNA 元件家族,最近作为一种潜在的新型调控源而受到关注,其中最引人注目的是它参与了增强子功能。尽管通过 RNA 聚合酶 III 转录的 Alu 会受到严格的表观遗传沉默,但人们早已知道它们的表达会在包括病毒感染在内的各种压力下增加。在这里,我们发现在原代人类成纤维细胞中,腺病毒小e1a通过促进与Alu结合的TFIIIC招募TFIIIB,触发了数百个单独Alu的去抑制。表观基因组图谱显示,e1a诱导的H3K27乙酰化减少,H3K4单甲基化增加,使被去抑制的Alus类似于蓄势待发的增强子。EP300/CBP乙酰转移酶、EP400染色质重塑因子以及YAP1和FOS转录因子在其上游区域的富集证实了e1a靶向Alu的增强子性质。e1a与EP400的物理相互作用对于Alu的去抑制至关重要,而EP400的消减又会导致Alu的去抑制消失。我们的数据表明,e1a以增强子Alu亚群为靶标,其转录激活需要EP400并由e1a-EP400相互作用介导,e1a可能参与了腺病毒对增强子活性的操纵。
Adenovirus small E1A directs activation of Alu transcription at YAP/TEAD- and AP-1-bound enhancers through interactions with the EP400 chromatin remodeler.
Alu retrotransposons, which form the largest family of mobile DNA elements in the human genome, have recently come to attention as a potential source of regulatory novelties, most notably by participating in enhancer function. Even though Alu transcription by RNA polymerase III is subjected to tight epigenetic silencing, their expression has long been known to increase in response to various types of stress, including viral infection. Here we show that, in primary human fibroblasts, adenovirus small e1a triggered derepression of hundreds of individual Alus by promoting TFIIIB recruitment by Alu-bound TFIIIC. Epigenome profiling revealed an e1a-induced decrease of H3K27 acetylation and increase of H3K4 monomethylation at derepressed Alus, making them resemble poised enhancers. The enhancer nature of e1a-targeted Alus was confirmed by the enrichment, in their upstream regions, of the EP300/CBP acetyltransferase, EP400 chromatin remodeler and YAP1 and FOS transcription factors. The physical interaction of e1a with EP400 was critical for Alu derepression, which was abrogated upon EP400 ablation. Our data suggest that e1a targets a subset of enhancer Alus whose transcriptional activation, which requires EP400 and is mediated by the e1a-EP400 interaction, may participate in the manipulation of enhancer activity by adenoviruses.
期刊介绍:
Nucleic Acids Research (NAR) is a scientific journal that publishes research on various aspects of nucleic acids and proteins involved in nucleic acid metabolism and interactions. It covers areas such as chemistry and synthetic biology, computational biology, gene regulation, chromatin and epigenetics, genome integrity, repair and replication, genomics, molecular biology, nucleic acid enzymes, RNA, and structural biology. The journal also includes a Survey and Summary section for brief reviews. Additionally, each year, the first issue is dedicated to biological databases, and an issue in July focuses on web-based software resources for the biological community. Nucleic Acids Research is indexed by several services including Abstracts on Hygiene and Communicable Diseases, Animal Breeding Abstracts, Agricultural Engineering Abstracts, Agbiotech News and Information, BIOSIS Previews, CAB Abstracts, and EMBASE.