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Por favor, use este identificador para citar o enlazar a este item: http://hdl.handle.net/10261/24712
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dc.contributor.authorGoeman, Frauke-
dc.contributor.authorAbad, María-
dc.contributor.authorSerrano, Manuel-
dc.contributor.authorPalmero, Ignacio-
dc.contributor.authorBaniahmad, Aria-
dc.date.accessioned2010-05-26T10:26:34Z-
dc.date.available2010-05-26T10:26:34Z-
dc.date.issued2005-01-
dc.identifier.citationMolecular and Cellular Biology 25(1): 422-431 (2005)en_US
dc.identifier.issn0270-7306-
dc.identifier.urihttp://hdl.handle.net/10261/24712-
dc.description10 pages, 7 figures.-- et al.en_US
dc.description.abstractING1 was identified as an inhibitor of growth and has been described as a tumor suppressor. Furthermore, the expression of ING1 is induced in senescent cells and antisense ING1 extends the proliferative life span of primary human fibroblasts. Cooperation of p33ING1 with p53 has been suggested to be an important function of ING1 in cell cycle control. Intriguingly, it has been shown that p33ING1 is associated with histone acetylation as well as with histone deacetylation function. Here we show that p33ING1 is a potent transcriptional silencer in various cell types. However, the silencing function is independent of the presence of p53. By use of deletion mutants two potent autonomous and transferable silencing domains were identified, but no evidence of an activation domain was found. The amino (N)-terminal silencing domain is sensitive to the histone deacetylase inhibitor trichostatin A (TSA) whereas the carboxy-terminal silencing function is resistant to TSA, suggesting that p33ING1 confers gene silencing through both HDAC-dependent and -independent mechanisms. Interestingly, the presence of oncogenic Ras, which is able to induce premature senescence, increases the p33ING1-mediated silencing function. Moreover, ING1-mediated silencing was reduced by coexpressing dominant-negative Ras or by treatment with the mitogen-activated protein kinase inhibitor PD98059 but not by treatment with SB203580, an inhibitor of the p38 pathway. In addition, we show that both silencing domains of ING1 are involved in cell cycle control, as measured by inhibition of colony formation of immortalized cells and by thymidine incorporation of primary human diploid fibroblasts (HDF). Interestingly, p33ING1 expression induces features of cellular senescence in HDFs.en_US
dc.description.sponsorshipPart of this work was supported by the Graduiertenkolleg 370 (F.G.). This work has been supported by grants from the Spanish Ministry of Education (SAF03-00801) and the Cooperative Cancer Network of the Spanish Ministry of Health.en_US
dc.format.extent713544 bytes-
dc.format.mimetypeapplication/pdf-
dc.language.isoengen_US
dc.publisherAmerican Society for Microbiologyen_US
dc.rightsclosedAccessen_US
dc.titleGrowth inhibition by the tumor suppressor p33ING1 in immortalized and primary cells: involvement of two silencing domains and effect of Rasen_US
dc.typeartículoen_US
dc.identifier.doi10.1128/MCB.25.1.422-431.2005-
dc.description.peerreviewedPeer revieweden_US
dc.relation.publisherversionhttp://dx.doi.org/10.1128/MCB.25.1.422-431.2005en_US
dc.identifier.pmid15601862-
dc.type.coarhttp://purl.org/coar/resource_type/c_6501es_ES
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.fulltextNo Fulltext-
item.cerifentitytypePublications-
item.openairetypeartículo-
item.languageiso639-1en-
item.grantfulltextnone-
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