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Tumor Suppressor SMAR1 Mediates Cyclin D1 Repression by Recruitment of the SIN3/Histone Deacetylase 1 Complex

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dc.contributor.author Rampalli, Shravanti
dc.contributor.author Pavithra, L
dc.contributor.author Bhatt, Altaf
dc.contributor.author Kundu, Tapas K
dc.contributor.author Chattopadhyay, Samit
dc.date.accessioned 2012-01-04T11:12:56Z
dc.date.available 2012-01-04T11:12:56Z
dc.date.issued 2005-10
dc.identifier 0270-7306 en_US
dc.identifier.citation Molecular And Cellular Biology 25(19), 8415-8429 (2005) en_US
dc.identifier.uri https://libjncir.jncasr.ac.in/xmlui/10572/139
dc.description.abstract Matrix attachment region binding proteins have been shown to play an important role in gene regulation by altering chromatin in a stage- and tissue-specific manner. Our previous studies report that SMAR1, a matrix-associated protein, regresses B16-F1-induced tumors in mice. Here we show SMAR1 targets the cyclin D1 promoter, a gene product whose dysregulation is attributed to breast malignancies. Our studies reveal that SMAR1 represses cyclin D1 gene expression, which can be reversed by small interfering RNA specific to SMAR1. We demonstrate that SMAR1 interacts with histone deacetylation complex 1, SIN3, and pocket retinoblastomas to form a multiprotein repressor complex. This interaction is mediated by the SMAR1(160-350) domain. Our data suggest SMAR1 recruits a repressor complex to the cyclin D1 promoter that results in deacetylation of chromatin at that locus, which spreads to a distance of at least the 5 kb studied upstream of the cyclin D1 promoter. Interestingly, we find that the high induction of cyclin D1 in breast cancer cell lines can be correlated to the decreased levels of SMAR1 in these lines. Our results establish the molecular mechanism exhibited by SMAR1 to regulate cyclin D1 by modification of chromatin. en_US
dc.description.uri http://dx.doi.org/10.1128/MCB.25.19.8415-8429.2005 en_US
dc.language.iso en en_US
dc.publisher American Society for Microbiology en_US
dc.rights © 2005 American Society for Microbiology en_US
dc.subject Histone Deacetylase en_US
dc.subject Gene-Expression en_US
dc.subject Transcriptional Repression en_US
dc.subject Breast-Cancer en_US
dc.subject Growth Arrest en_US
dc.subject P53 en_US
dc.subject Phosphorylation en_US
dc.subject Overexpression en_US
dc.subject Localization en_US
dc.subject Progression en_US
dc.title Tumor Suppressor SMAR1 Mediates Cyclin D1 Repression by Recruitment of the SIN3/Histone Deacetylase 1 Complex en_US
dc.type Article en_US


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