Ing1 Mediates p53 Accumulation and Chromatin Modification in Response to Oncogenic Stress

Abad, María; Menéndez, Camino; Füchtbauer, Annette; Serrano, Manuel; Füchtbauer, Ernst‐Martin; Palmero, Ignacio

doi:10.1074/jbc.m701639200

Cited by 24 publications

(25 citation statements)

References 41 publications

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“…This finding indicates a predominant role for Ing1 as a transcriptional repressor, in agreement with previous biochemical studies (16,18). As an internal validation of the experiment, we found that the signal for the Ing1 probe was reduced ∼10-fold in the Ing1-mutant fibroblasts (Ing1-mutant/wildtype ratio, 0.11; P = 0.0004), consistent with our previous characterization of the expression of the Ing1 locus in this cell type (24). In addition, we found that the expression of the other Ing loci is not significantly altered in Ing1-mutant cells, with the possible exception of Ing5 (Supplementary Table S1).…”

Section: Resultssupporting

confidence: 80%

“…The Ing1-deficient MEFs we have used in this study display a dramatic reduction (>90%) in the expression of all the transcripts of the locus, as a consequence of the insertion of a BetaGeo genetrap cassette. The levels of the p33ING1 protein (the only ING1 peptide detectable in MEFs) are also reduced to the same extent (24). Of the 37,898 probes, representing >30,000 genes, present in the array, we found a significantly differential expression associated to Ing1 status (at least 2-fold change, see Materials and Methods) for 466 of them (∼1.2% of the total).…”

Section: Resultsmentioning

confidence: 84%

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Regulation of the MicroRNA Processor DGCR8 by the Tumor Suppressor ING1

et al. 2010

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The ING family of tumor suppressor proteins controls several cellular functions relevant to antitumor protection, such as cell cycle control, apoptosis, senescence, or migration. ING proteins are functionally linked to the p53 pathway, and they participate in transcriptional control via the recognition of histone marks and recruitment of protein complexes with chromatin-modifying activity to specific promoters. Here, we have investigated the global effect of ING1 in gene regulation through genome-wide analysis of expression profiles in primary embryonic fibroblasts deficient for the Ing1 locus. We find that Ing1 has a predominant role as transcriptional repressor in this setting, affecting the expression of genes involved in a variety of cellular functions. Within the subset of genes showing differential expression, we have identified DGCR8, a protein involved in the early steps of microRNA biogenesis. We show that ING1 binds to the DGCR8 promoter and controls its transcription through chromatin regulation. We also find that ING1 and DGCR8 can cooperate in restraining proliferation. In summary, this study reveals a novel connection between ING1 and a regulator of microRNA biogenesis and identifies new links between tumor suppressor proteins and the microRNA machinery. Cancer Res; 70(5); 1866-74. ©2010 AACR.

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Section: Resultssupporting

confidence: 80%

Section: Resultsmentioning

confidence: 84%

Regulation of the MicroRNA Processor DGCR8 by the Tumor Suppressor ING1

et al. 2010

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“…Consistent with this idea and our current data, it was recently reported that deletion of the Ing1 locus from murine cells impairs Ras-induced senescence (Abad et al, 2007). Hints as to how INGl, and the INGla splice isoform in particular, contribute to establishment of a senescent state are provided by the ability of INGla to repress expression of some genes such as PCNA which is required for growth while inducing others such as the pl6 and pRb which are associated with the induction of senescence, upon ectopic expression.…”

Section: Discussionsupporting

confidence: 82%

ING1a expression increases during replicative senescence and induces a senescent phenotype

Soliman

Berardi

Pastyryeva³

et al. 2008

Aging Cell

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“…Neuronal gene expression, like other transcriptional processes, is modulated by a dynamic process of chromatin modifications (3)(4)(5). According to the histone code hypothesis, different modifications of histones at a particular promoter region, alone or in combination, define a specific epigenetic state that balances between gene activation and gene silencing (6,7). Although there are exceptions, histone hyperacetylation at promoters generally indicates an increase in gene activity, whereas hypoacetylation usually marks a decrease in activity (8).…”

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confidence: 99%

Stress-induced epigenetic transcriptional memory of acetylcholinesterase by HDAC4

Sailaja

Cohen-Carmon²,

Zimmerman

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

105

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Stress induces long-lasting changes in neuronal gene expression and cholinergic neurotransmission, but the underlying mechanism(s) are incompletely understood. Here, we report that chromatin structure and histone modifications are causally involved in this transcriptional memory. Specifically, the AChE gene encoding the acetylcholine-hydrolyzing enzyme acetylcholinesterase is known to undergo long-lasting transcriptional and alternative splicing changes after stress. In mice subjected to stress, we identified two alternative 5′ exons that were down-regulated after stress in the hippocampus, accompanied by reduced acetylation and elevated trimethylation of H3K9 at the corresponding promoter. These effects were reversed completely by daily administration of the histone deacetylase (HDAC) inhibitor sodium butyrate for 1 wk after stress. H3K9 hypoacetylation was associated with a selective, sodium butyrate-reversible promoter accumulation of HDAC4. Hippocampal suppression of HDAC4 in vivo completely abolished the long-lasting AChE-related and behavioral stress effects. Our findings demonstrate long-lasting stress-inducible changes in AChE's promoter choices, identify the chromatin changes that support this long-term transcriptional memory, and reveal HDAC4 as a mediator of these effects in the hippocampus.HDAC inhibitors | ChIP | chromatin immunoprecipitation | histone methylation | histone acetylation

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Ing1 Mediates p53 Accumulation and Chromatin Modification in Response to Oncogenic Stress

Cited by 24 publications

References 41 publications

Regulation of the MicroRNA Processor DGCR8 by the Tumor Suppressor ING1

Regulation of the MicroRNA Processor DGCR8 by the Tumor Suppressor ING1

ING1a expression increases during replicative senescence and induces a senescent phenotype

Stress-induced epigenetic transcriptional memory of acetylcholinesterase by HDAC4

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