Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress

Master regulator protein p53, popularly known as the “guardian of genome” is the hub for regulation of diverse cellular pathways. Depending on the cell type and severity of DNA damage, p53 protein mediates cell cycle arrest or apoptosis, besides activating DNA repair, which is apparently achieved by...

Descripción completa

Detalles Bibliográficos
Autores principales: Bansal, Nidhi, Kadamb, Rama, Mittal, Shilpi, Vig, Leena, Sharma, Raisha, Dwarakanath, Bilikere S., Saluja, Daman
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3197607/
https://www.ncbi.nlm.nih.gov/pubmed/22028823
http://dx.doi.org/10.1371/journal.pone.0026156
_version_ 1782214338070708224
author Bansal, Nidhi
Kadamb, Rama
Mittal, Shilpi
Vig, Leena
Sharma, Raisha
Dwarakanath, Bilikere S.
Saluja, Daman
author_facet Bansal, Nidhi
Kadamb, Rama
Mittal, Shilpi
Vig, Leena
Sharma, Raisha
Dwarakanath, Bilikere S.
Saluja, Daman
author_sort Bansal, Nidhi
collection PubMed
description Master regulator protein p53, popularly known as the “guardian of genome” is the hub for regulation of diverse cellular pathways. Depending on the cell type and severity of DNA damage, p53 protein mediates cell cycle arrest or apoptosis, besides activating DNA repair, which is apparently achieved by regulation of its target genes, as well as direct interaction with other proteins. p53 is known to repress target genes via multiple mechanisms one of which is via recruitment of chromatin remodelling Sin3/HDAC1/2 complex. Sin3 proteins (Sin3A and Sin3B) regulate gene expression at the chromatin-level by serving as an anchor onto which the core Sin3/HDAC complex is assembled. The Sin3/HDAC co-repressor complex can be recruited by a large number of DNA-binding transcription factors. Sin3A has been closely linked to p53 while Sin3B is considered to be a close associate of E2Fs. The theme of this study was to establish the role of Sin3B in p53-mediated gene repression. We demonstrate a direct protein-protein interaction between human p53 and Sin3B (hSin3B). Amino acids 1–399 of hSin3B protein are involved in its interaction with N-terminal region (amino acids 1–108) of p53. Genotoxic stress induced by Adriamycin treatment increases the levels of hSin3B that is recruited to the promoters of p53-target genes (HSPA8, MAD1 and CRYZ). More importantly recruitment of hSin3B and repression of the three p53-target promoters upon Adriamycin treatment were observed only in p53(+/+) cell lines. Additionally an increased tri-methylation of the H3K9 residue at the promoters of HSPA8 and CRYZ was also observed following Adriamycin treatment. The present study highlights for the first time the essential role of Sin3B as an important associate of p53 in mediating the cellular responses to stress and in the transcriptional repression of genes encoding for heat shock proteins or proteins involved in regulation of cell cycle and apoptosis.
format Online
Article
Text
id pubmed-3197607
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-31976072011-10-25 Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress Bansal, Nidhi Kadamb, Rama Mittal, Shilpi Vig, Leena Sharma, Raisha Dwarakanath, Bilikere S. Saluja, Daman PLoS One Research Article Master regulator protein p53, popularly known as the “guardian of genome” is the hub for regulation of diverse cellular pathways. Depending on the cell type and severity of DNA damage, p53 protein mediates cell cycle arrest or apoptosis, besides activating DNA repair, which is apparently achieved by regulation of its target genes, as well as direct interaction with other proteins. p53 is known to repress target genes via multiple mechanisms one of which is via recruitment of chromatin remodelling Sin3/HDAC1/2 complex. Sin3 proteins (Sin3A and Sin3B) regulate gene expression at the chromatin-level by serving as an anchor onto which the core Sin3/HDAC complex is assembled. The Sin3/HDAC co-repressor complex can be recruited by a large number of DNA-binding transcription factors. Sin3A has been closely linked to p53 while Sin3B is considered to be a close associate of E2Fs. The theme of this study was to establish the role of Sin3B in p53-mediated gene repression. We demonstrate a direct protein-protein interaction between human p53 and Sin3B (hSin3B). Amino acids 1–399 of hSin3B protein are involved in its interaction with N-terminal region (amino acids 1–108) of p53. Genotoxic stress induced by Adriamycin treatment increases the levels of hSin3B that is recruited to the promoters of p53-target genes (HSPA8, MAD1 and CRYZ). More importantly recruitment of hSin3B and repression of the three p53-target promoters upon Adriamycin treatment were observed only in p53(+/+) cell lines. Additionally an increased tri-methylation of the H3K9 residue at the promoters of HSPA8 and CRYZ was also observed following Adriamycin treatment. The present study highlights for the first time the essential role of Sin3B as an important associate of p53 in mediating the cellular responses to stress and in the transcriptional repression of genes encoding for heat shock proteins or proteins involved in regulation of cell cycle and apoptosis. Public Library of Science 2011-10-20 /pmc/articles/PMC3197607/ /pubmed/22028823 http://dx.doi.org/10.1371/journal.pone.0026156 Text en Bansal et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Bansal, Nidhi
Kadamb, Rama
Mittal, Shilpi
Vig, Leena
Sharma, Raisha
Dwarakanath, Bilikere S.
Saluja, Daman
Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress
title Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress
title_full Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress
title_fullStr Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress
title_full_unstemmed Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress
title_short Tumor Suppressor Protein p53 Recruits Human Sin3B/HDAC1 Complex for Down-Regulation of Its Target Promoters in Response to Genotoxic Stress
title_sort tumor suppressor protein p53 recruits human sin3b/hdac1 complex for down-regulation of its target promoters in response to genotoxic stress
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3197607/
https://www.ncbi.nlm.nih.gov/pubmed/22028823
http://dx.doi.org/10.1371/journal.pone.0026156
work_keys_str_mv AT bansalnidhi tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress
AT kadambrama tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress
AT mittalshilpi tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress
AT vigleena tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress
AT sharmaraisha tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress
AT dwarakanathbilikeres tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress
AT salujadaman tumorsuppressorproteinp53recruitshumansin3bhdac1complexfordownregulationofitstargetpromotersinresponsetogenotoxicstress

Ejemplares similares