HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages

B lymphopoiesis is the result of several cell-commitment, lineage-choice, and differentiation processes. Every differentiation step is characterized by the activation of a new, lineage-specific, genetic program and the extinction of the previous one. To date, the central role of specific transcripti...

Descripción completa

Detalles Bibliográficos
Autores principales: Barneda-Zahonero, Bruna, Román-González, Lidia, Collazo, Olga, Rafati, Haleh, Islam, Abul B. M. M. K., Bussmann, Lars H., di Tullio, Alessandro, De Andres, Luisa, Graf, Thomas, López-Bigas, Núria, Mahmoudi, Tokameh, Parra, Maribel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3656156/
https://www.ncbi.nlm.nih.gov/pubmed/23696748
http://dx.doi.org/10.1371/journal.pgen.1003503
_version_ 1782269992793800704
author Barneda-Zahonero, Bruna
Román-González, Lidia
Collazo, Olga
Rafati, Haleh
Islam, Abul B. M. M. K.
Bussmann, Lars H.
di Tullio, Alessandro
De Andres, Luisa
Graf, Thomas
López-Bigas, Núria
Mahmoudi, Tokameh
Parra, Maribel
author_facet Barneda-Zahonero, Bruna
Román-González, Lidia
Collazo, Olga
Rafati, Haleh
Islam, Abul B. M. M. K.
Bussmann, Lars H.
di Tullio, Alessandro
De Andres, Luisa
Graf, Thomas
López-Bigas, Núria
Mahmoudi, Tokameh
Parra, Maribel
author_sort Barneda-Zahonero, Bruna
collection PubMed
description B lymphopoiesis is the result of several cell-commitment, lineage-choice, and differentiation processes. Every differentiation step is characterized by the activation of a new, lineage-specific, genetic program and the extinction of the previous one. To date, the central role of specific transcription factors in positively regulating these distinct differentiation processes to acquire a B cell–specific genetic program is well established. However, the existence of specific transcriptional repressors responsible for the silencing of lineage inappropriate genes remains elusive. Here we addressed the molecular mechanism behind repression of non-lymphoid genes in B cells. We report that the histone deacetylase HDAC7 was highly expressed in pre-B cells but dramatically down-regulated during cellular lineage conversion to macrophages. Microarray analysis demonstrated that HDAC7 re-expression interfered with the acquisition of the gene transcriptional program characteristic of macrophages during cell transdifferentiation; the presence of HDAC7 blocked the induction of key genes for macrophage function, such as immune, inflammatory, and defense response, cellular response to infections, positive regulation of cytokines production, and phagocytosis. Moreover, re-introduction of HDAC7 suppressed crucial functions of macrophages, such as the ability to phagocytose bacteria and to respond to endotoxin by expressing major pro-inflammatory cytokines. To gain insight into the molecular mechanisms mediating HDAC7 repression in pre-B cells, we undertook co-immunoprecipitation and chromatin immunoprecipitation experimental approaches. We found that HDAC7 specifically interacted with the transcription factor MEF2C in pre-B cells and was recruited to MEF2 binding sites located at the promoters of genes critical for macrophage function. Thus, in B cells HDAC7 is a transcriptional repressor of undesirable genes. Our findings uncover a novel role for HDAC7 in maintaining the identity of a particular cell type by silencing lineage-inappropriate genes.
format Online
Article
Text
id pubmed-3656156
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-36561562013-05-21 HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages Barneda-Zahonero, Bruna Román-González, Lidia Collazo, Olga Rafati, Haleh Islam, Abul B. M. M. K. Bussmann, Lars H. di Tullio, Alessandro De Andres, Luisa Graf, Thomas López-Bigas, Núria Mahmoudi, Tokameh Parra, Maribel PLoS Genet Research Article B lymphopoiesis is the result of several cell-commitment, lineage-choice, and differentiation processes. Every differentiation step is characterized by the activation of a new, lineage-specific, genetic program and the extinction of the previous one. To date, the central role of specific transcription factors in positively regulating these distinct differentiation processes to acquire a B cell–specific genetic program is well established. However, the existence of specific transcriptional repressors responsible for the silencing of lineage inappropriate genes remains elusive. Here we addressed the molecular mechanism behind repression of non-lymphoid genes in B cells. We report that the histone deacetylase HDAC7 was highly expressed in pre-B cells but dramatically down-regulated during cellular lineage conversion to macrophages. Microarray analysis demonstrated that HDAC7 re-expression interfered with the acquisition of the gene transcriptional program characteristic of macrophages during cell transdifferentiation; the presence of HDAC7 blocked the induction of key genes for macrophage function, such as immune, inflammatory, and defense response, cellular response to infections, positive regulation of cytokines production, and phagocytosis. Moreover, re-introduction of HDAC7 suppressed crucial functions of macrophages, such as the ability to phagocytose bacteria and to respond to endotoxin by expressing major pro-inflammatory cytokines. To gain insight into the molecular mechanisms mediating HDAC7 repression in pre-B cells, we undertook co-immunoprecipitation and chromatin immunoprecipitation experimental approaches. We found that HDAC7 specifically interacted with the transcription factor MEF2C in pre-B cells and was recruited to MEF2 binding sites located at the promoters of genes critical for macrophage function. Thus, in B cells HDAC7 is a transcriptional repressor of undesirable genes. Our findings uncover a novel role for HDAC7 in maintaining the identity of a particular cell type by silencing lineage-inappropriate genes. Public Library of Science 2013-05-16 /pmc/articles/PMC3656156/ /pubmed/23696748 http://dx.doi.org/10.1371/journal.pgen.1003503 Text en © 2013 Barneda-Zahonero 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
Barneda-Zahonero, Bruna
Román-González, Lidia
Collazo, Olga
Rafati, Haleh
Islam, Abul B. M. M. K.
Bussmann, Lars H.
di Tullio, Alessandro
De Andres, Luisa
Graf, Thomas
López-Bigas, Núria
Mahmoudi, Tokameh
Parra, Maribel
HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages
title HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages
title_full HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages
title_fullStr HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages
title_full_unstemmed HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages
title_short HDAC7 Is a Repressor of Myeloid Genes Whose Downregulation Is Required for Transdifferentiation of Pre-B Cells into Macrophages
title_sort hdac7 is a repressor of myeloid genes whose downregulation is required for transdifferentiation of pre-b cells into macrophages
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3656156/
https://www.ncbi.nlm.nih.gov/pubmed/23696748
http://dx.doi.org/10.1371/journal.pgen.1003503
work_keys_str_mv AT barnedazahonerobruna hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT romangonzalezlidia hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT collazoolga hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT rafatihaleh hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT islamabulbmmk hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT bussmannlarsh hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT ditullioalessandro hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT deandresluisa hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT grafthomas hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT lopezbigasnuria hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT mahmouditokameh hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages
AT parramaribel hdac7isarepressorofmyeloidgeneswhosedownregulationisrequiredfortransdifferentiationofprebcellsintomacrophages

Ejemplares similares