Methyltransferase Recruitment and DNA Hypermethylation of Target Promoters by an Oncogenic Transcription Factor

Croce, Luciano Di; Raker, Veronica A.; Corsaro, Massimo; Fazi, Francesco; Fanelli, Mirco; Faretta, Mario; Fuks, François; Coco, Francesco Lo; Kouzarides, Tony; Nervi, Clara; Minucci, Saverio; Pelicci, Pier Giuseppe

doi:10.1126/science.1065173

Cited by 738 publications

(572 citation statements)

References 23 publications

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“…A few genetic mutations involving RARa were indeed reported in cancer cells and found associated with either RARb2 or Cyp26a1 downregulation. PML-RARa, an oncogenic protein associated with acute promyelocitic leukemia, which leads to block of myeloid maturation both in vitro and in vivo (He et al, 1998;Grignani et al, 2000), was shown to induce epigenetic repression of RARb2 in the presence of DNA methylation (Di Croce et al, 2002). However, we show that in embryocarcinoma cells RARb2 silencing can occur also by virtue of an accumulation of repressive Cyp26a1 is epigenetically regulated by retinoic acid receptors S Pozzi et al chromatin changes in the absence of DNA methylation.…”

Section: Discussionmentioning

confidence: 99%

RAR-mediated epigenetic control of the cytochrome P450 Cyp26a1 in embryocarcinoma cells

et al. 2005

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Section: Discussionmentioning

confidence: 99%

RAR-mediated epigenetic control of the cytochrome P450 Cyp26a1 in embryocarcinoma cells

et al. 2005

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“…For example, activation of RAS [MacLeod et al, 1995], down regulation of Rb [Slack et al, 1999], or upregulation of the Wnt signaling pathway [Campbell and Szyf, 2003] leads to increased expression of DNMT1. Certain oncogenes could target DNMT to tumor suppressor genes and thus bring about regional hypermethylation [Fuks et al, 2001;Di Croce et al, 2002;Brenner et al, 2005;Vire et al, 2006]. An interesting possibility is that aberrant DNA methylation of cancer related genes could also come about through activation of signaling pathway by different environmental exposures, which might also include social exposures.…”

Section: Epigenetic Plasticity and Late Onset Pathologymentioning

confidence: 99%

The social environment and the epigenome

Szyf

McGowan

Meaney

2007

Environ and Mol Mutagen

450

220

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The genome is programmed by the epigenome. Two of the fundamental components of the epigenome are chromatin structure and covalent modification of the DNA molecule itself by methylation. DNA methylation patterns are sculpted during development and it has been a long held belief that they remain stable after birth in somatic tissues. Recent data suggest that DNA methylation is dynamic later in life in postmitotic cells such as neurons and thus potentially responsive to different environmental stimuli throughout life. We hypothesize a mechanism linking the social environment early in life and long-term epigenetic programming of behavior and responsiveness to stress and health status later in life. We will also discuss the prospect that the epigenetic equilibrium remains responsive throughout life and that therefore environmental triggers could play a role in generating interindividual differences in human behavior later in life. We speculate that exposures to different environmental toxins alters long-established epigenetic programs in the brain as well as other tissues leading to lateonset disease. Environ. Mol. Mutagen. 49:46-60, 2008. V V C 2007 Wiley-Liss, Inc.

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“…After induction with 100 mM Zn for 12 h, cells were treated with 1 ng/ml 1a,25-dihydroxyvitamin D 3 for another 36 h. Cells were then analysed for CD14 expression by flow cytometry as described (Di Croce et al, 2002).…”

Section: Analysis Of Cell Differentiationmentioning

confidence: 99%