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The adenoviral E1A N-terminal domain represses MYC transcription in human cancer cells by targeting both p300 and TRRAP and inhibiting MYC promoter acetylation of H3K18 and H4K16

机译：腺病毒E1A N末端结构域通过靶向p300和TRRAP并抑制H3K18和H4K16的MYC启动子乙酰化来抑制人癌细胞中的MYC转录

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Human cancers frequently arise from increased expression of proto-oncogenes, such as MYC and HER2. Understanding the cellular pathways regulating the transcription and expression of proto-oncogenes is important for targeted therapies for cancer treatment. Adenoviral (Ad) E1A 243R (243 aa residues) is a viral oncoprotein that interacts with key regulators of gene transcription and cell proliferation. We have shown previously that the 80 amino acid N-terminal transcriptional repression domain of E1A 243R (E1A 1-80) can target the histone acetyltransferase (HAT) p300 and repress HER2 in the HER2-overexpressing human breast cancer cell line SKBR3. Expression of E1A 1-80 induces death of SKBR3 and other cancer cell lines. In this study, we performed total cell RNA sequence analysis and identified MYC as the regulatory gene for cellular proliferation most strongly repressed by E1A 1-80. By RT-quantitative PCR analysis we show that repression of MYC in SKBR3 cells occurs early after expression of E1A 1-80, suggesting that MYC may be an early responder of E1A 1-80-mediated transcriptional repression. Of interest, while E1A 1-80 repression of MYC occurs in all eight human cancer cell lines examined, repression of HER2 is cell-type dependent. We demonstrate by ChIP analysis that MYC transcriptional repression by E1A 1-80 is associated with inhibition of acetylation of H3K18 and H4K16 on the MYC promoter, as well as inhibition of RNA Pol II binding to the MYC promoter. Deletion mutant analysis of E1A 1-80 suggests that both p300/CBP and TRRAP are involved in E1A 1-80 repression of MYC transcription. Further, E1A 1-80 interaction with p300/CBP and TRRAP is correlated with inhibition of H3K18 and H4K16 acetylation on the MYC promoter, respectively. Our results indicate that E1A 1-80 may target two important pathways for histone modification to repress transcription in human cancer cells.

机译：人类癌症通常源于原癌基因（例如MYC和HER2）的表达增加。理解调节原癌基因转录和表达的细胞途径对于癌症治疗的靶向治疗很重要。腺病毒（Ad）E1A 243R（243个氨基酸残基）是一种病毒癌蛋白，与基因转录和细胞增殖的关键调节因子相互作用。先前我们已经表明，E1A 243R的80个氨基酸的N末端转录抑制结构域（E1A 1-80）可以靶向组蛋白乙酰转移酶（HAT）p300，并抑制过表达HER2的人乳腺癌细胞SKBR3中的HER2。 E1A 1-80的表达诱导SKBR3和其他癌细胞系的死亡。在这项研究中，我们进行了总细胞RNA序列分析，并将MYC鉴定为E1A 1-80最强烈抑制的细胞增殖调控基因。通过RT定量PCR分析，我们显示SKBR3细胞中MYC的抑制发生在E1A 1-80表达后的早期，这表明MYC可能是E1A 1-80介导的转录抑制的早期应答者。有趣的是，虽然在检查的所有八种人类癌细胞系中均发生MYC的E1A 1-80抑制，但HER2的抑制却依赖于细胞类型。我们通过ChIP分析证明，E1A 1-80对MYC转录的抑制作用与MYC启动子上H3K18和H4K16乙酰化的抑制有关，以及与MYC启动子结合的RNA Pol II的抑制。 E1A 1-80的缺失突变分析表明，p300 / CBP和TRRAP均参与MYC转录的E1A 1-80抑制。此外，E1A 1-80与p300 / CBP和TRRAP的相互作用分别与抑制MYC启动子上的H3K18和H4K16乙酰化有关。我们的结果表明，E1A 1-80可能靶向组蛋白修饰的两个重要途径，以抑制人类癌细胞中的转录。

著录项

期刊名称 Genes Cancer
作者
Ling-Jun Zhao; Paul M. Loewenstein; Maurice Green;
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作者单位

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年(卷),期 2016(7),3-4
年度 2016
页码 98–109
总页数 12
原文格式 PDF
正文语种
中图分类肿瘤学 ;
关键词
adenoviral E1A 1-80 transcriptional repression MYC HER2 H3K18Ac H4K16Ac p300/CBP TRRAP;

机译：腺病毒E1A 1-80;转录抑制;MYC;HER2;H3K18Ac;H4K16Ac;p300 / CBP;TRRAP;

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专利

1. Adenovirus E1A TRRAP-targeting domain-mediated enhancement of MYC association with the NuA4 complex activates a panel of MYC target genes enriched for gene expression and ribosome biogenesis [J] . Ling-Jun Zhao, Paul M. Loewenstein, Maurice Green Virology . 2017 ,第期

机译：腺病毒E1A TRRAP靶向域介导的MYC与NUA4复合物的增强激活了富含基因表达和核糖体生物发生的MYC靶基因的面板
2. Dual Regulation of c-Myc by p300 via Acetylation-Dependent Control of Myc Protein Turnover and Coactivation of Myc-Induced Transcription [J] . Francesco Faiola, Xiaohui Liu, Szuying Lo, Molecular and Cellular Biology . 2005 ,第23期

机译：p300通过乙酰化依赖控制Myc蛋白周转和共激活Myc诱导的转录的p300双重调控c-Myc。
3. The human cut homeodomain protein represses transcription from the c-myc promoter. [J] . D Dufort, A Nepveu Molecular and Cellular Biology . 1994 ,第6期

机译：人切割的同源结构域蛋白抑制了c-myc启动子的转录。
4. IL-5 Inhibits Apoptosis by Upregulation of c-myc Expression in Human Hematopoietic Cells [C] . SHU-HUI JUAN, JEFFREY JONG-YOUNG YEN, HORNG-MO LEE, Asian Society for Mitochondrial Research and Medicine . 2005

机译：IL-5通过造血细胞中的C-MYC表达的上调抑制细胞凋亡
5. Analysis of c -MYC target gene specificity in living cells using the CAD promoter as a model system. [D] . Boyd, Kathryn Elizabeth. 1999

机译：使用CAD启动子作为模型系统分析活细胞中c -MYC靶基因的特异性。
6. Enhanced MYC association with the NuA4 histone acetyltransferase complex mediated by the adenovirus E1A N-terminal domain activates a subset of MYC target genes highly expressed in cancer cells [O] . Ling-Jun Zhao, Paul M. Loewenstein, Maurice Green 2017

机译：增强的MYC与腺病毒E1A N端域介导的NuA4组蛋白乙酰转移酶复合物的结合激活了在癌细胞中高度表达的MYC目标基因的一个子集
7. The adenoviral E1A N-terminal domain represses MYC transcription in human cancer cells by targeting both p300 and TRRAP and inhibiting MYC promoter acetylation of H3K18 and H4K16 [O] . Ling-Jun Zhao, Paul M. Loewenstein, Maurice Green 2016

机译：腺病毒E1a n-末端域通过靶向P300和TRRAP并抑制H3K18和H4K16的MYC启动子乙酰化，抑制人癌细胞中的MYC转录
8. High-Content FRET-FLIM Screening in Inhibitors of Oncogenic Transcription by C-Myc in Breast Cancer [R] . Andrews, D., Penn, L. 2009

机译：高密度FRET-FLIm筛选C-myc在乳腺癌中的致癌转录抑制剂

The adenoviral E1A N-terminal domain represses MYC transcription in human cancer cells by targeting both p300 and TRRAP and inhibiting MYC promoter acetylation of H3K18 and H4K16

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