c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study

c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study

Relationships between c-Rel and GCB-DLBCLs remain unclear. We found that strong c-Rel DNA-binding activity was mostly found in GCBs on two independent series of 48 DLBCLs and 66 DLBCLs, the latter issued from the GHEDI series. c-Rel DNA-binding activity was associated with increased REL mRNA express...

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Main Authors: Nathalie Faumont, Oussama Taoui, Davi Collares, Jean-Philippe Jais, Karen Leroy, Léa Prévaud, Fabrice Jardin, Thierry J. Molina, Christiane Copie-Bergman, Barbara Petit, Marie-Pierre Gourin, Dominique Bordessoule, Danielle Troutaud, Véronique Baud, Jean Feuillard
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-04-01
Series:Frontiers in Oncology
Subjects:
NF-kappaB
DNA binding activity
c-Rel
germinal center B-cell–diffuse large B-cell lymphoma
genetic alterations
Online Access:https://www.frontiersin.org/articles/10.3389/fonc.2021.638897/full
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language English
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author Nathalie Faumont
Oussama Taoui
Davi Collares
Jean-Philippe Jais
Karen Leroy
Léa Prévaud
Fabrice Jardin
Thierry J. Molina
Thierry J. Molina
Christiane Copie-Bergman
Barbara Petit
Marie-Pierre Gourin
Dominique Bordessoule
Dominique Bordessoule
Danielle Troutaud
Véronique Baud
Jean Feuillard
spellingShingle Nathalie Faumont
Oussama Taoui
Davi Collares
Jean-Philippe Jais
Karen Leroy
Léa Prévaud
Fabrice Jardin
Thierry J. Molina
Thierry J. Molina
Christiane Copie-Bergman
Barbara Petit
Marie-Pierre Gourin
Dominique Bordessoule
Dominique Bordessoule
Danielle Troutaud
Véronique Baud
Jean Feuillard
c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study
Frontiers in Oncology
NF-kappaB
DNA binding activity
c-Rel
germinal center B-cell–diffuse large B-cell lymphoma
genetic alterations
author_facet Nathalie Faumont
Oussama Taoui
Davi Collares
Jean-Philippe Jais
Karen Leroy
Léa Prévaud
Fabrice Jardin
Thierry J. Molina
Thierry J. Molina
Christiane Copie-Bergman
Barbara Petit
Marie-Pierre Gourin
Dominique Bordessoule
Dominique Bordessoule
Danielle Troutaud
Véronique Baud
Jean Feuillard
author_sort Nathalie Faumont
title c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study
title_short c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study
title_full c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study
title_fullStr c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study
title_full_unstemmed c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA Study
title_sort c-rel is the pivotal nf-κb subunit in germinal center diffuse large b-cell lymphoma: a lysa study
publisher Frontiers Media S.A.
series Frontiers in Oncology
issn 2234-943X
publishDate 2021-04-01
description Relationships between c-Rel and GCB-DLBCLs remain unclear. We found that strong c-Rel DNA-binding activity was mostly found in GCBs on two independent series of 48 DLBCLs and 66 DLBCLs, the latter issued from the GHEDI series. c-Rel DNA-binding activity was associated with increased REL mRNA expression. Extending the study to the whole GHEDI and Lenz DLBCL published series of 202 and 233 cases, it was found that the c-Rel gene expression profile (GEP) overlapped partially (12%) but only with the GCB GEP and not with the GEP of ABC-DLBCLs. Cases with both overexpression of REL mRNA and c-Rel GEP were defined as those having a c-Rel signature. These cases were GCBs in 88 and 83% of the GHEDI or Lenz’s DLBCL series respectively. The c-Rel signature was also associated with various recurrent GCB-DLBCL genetic events, including REL gains, BCL2 translocation, MEF2B, EZH2, CREBBP, and TNFRSF14 mutations and with the EZB GCB genetic subtype. By CGH array, the c-Rel signature was specifically correlated with 2p15-16.1 amplification that includes XPO1, BCL11A, and USP34 and with the 22q11.22 deletion that covers IGLL5 and PRAME. The total number of gene copy number aberrations, so-called genomic imbalance complexity, was decreased in cases with the c-Rel signature. These cases exhibited a better overall survival. Functionally, overexpression of c-Rel induced its constitutive nuclear localization and protected cells against apoptosis while its repression tended to increase cell death. These results show that, clinically and biologically, c-Rel is the pivotal NF-κB subunit in the GCB-DLBCL subgroup. Functionally, c-Rel overexpression could directly promote DLBCL tumorigenesis without need for further activation signals.
topic NF-kappaB
DNA binding activity
c-Rel
germinal center B-cell–diffuse large B-cell lymphoma
genetic alterations
url https://www.frontiersin.org/articles/10.3389/fonc.2021.638897/full
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spelling doaj-cc5e9e2c17bf4d2bb3dc4179c7dae4102021-04-20T15:16:15ZengFrontiers Media S.A.Frontiers in Oncology2234-943X2021-04-011110.3389/fonc.2021.638897638897c-Rel Is the Pivotal NF-κB Subunit in Germinal Center Diffuse Large B-Cell Lymphoma: A LYSA StudyNathalie Faumont0Oussama Taoui1Davi Collares2Jean-Philippe Jais3Karen Leroy4Léa Prévaud5Fabrice Jardin6Thierry J. Molina7Thierry J. Molina8Christiane Copie-Bergman9Barbara Petit10Marie-Pierre Gourin11Dominique Bordessoule12Dominique Bordessoule13Danielle Troutaud14Véronique Baud15Jean Feuillard16CNRS UMR-7276, INSERM U1262, CRIBL, University of Limoges, and Hematology Laboratory of Dupuytren Hospital University Center (CHU) of Limoges, Limoges, FranceCNRS UMR-7276, INSERM U1262, CRIBL, University of Limoges, and Hematology Laboratory of Dupuytren Hospital University Center (CHU) of Limoges, Limoges, FranceUniversité de Paris, NF-κappaB, Differentiation and Cancer, Paris, FranceBiostatistics Department, Imagine Institute, Paris, FranceUMRS1138, Centre de Recherche des Cordeliers, Paris Descartes University, CARPEM, Department of Genetics and Molecular Biology, Cochin Hospital, Assistance Publique Hôpitaux de Paris, Paris, FranceCNRS UMR-7276, INSERM U1262, CRIBL, University of Limoges, and Hematology Laboratory of Dupuytren Hospital University Center (CHU) of Limoges, Limoges, FranceInserm U1245 and Department of Henri-Becquerel Hematology Center and Normandie Univ UNIROUEN, Rouen, FranceUniversité de Paris, NF-κappaB, Differentiation and Cancer, Paris, FrancePathology Department, Necker Hospital, Assistance Publique Hôpitaux de Paris (AP-HP), Paris, FranceIMRB-Inserm U955, AP-HP Henri-Mondor Hospital, Créteil, FrancePathology Department, CHU of Limoges, Limoges, FranceRegional Reference Structure of Limousin Lymphomas, Clinical Hematology Department, CHU of Limoges, Limoges, FranceCNRS UMR-7276, INSERM U1262, CRIBL, University of Limoges, and Hematology Laboratory of Dupuytren Hospital University Center (CHU) of Limoges, Limoges, FranceRegional Reference Structure of Limousin Lymphomas, Clinical Hematology Department, CHU of Limoges, Limoges, France0EA3842, CAPTuR, University of Limoges, Limoges, FranceUniversité de Paris, NF-κappaB, Differentiation and Cancer, Paris, FranceCNRS UMR-7276, INSERM U1262, CRIBL, University of Limoges, and Hematology Laboratory of Dupuytren Hospital University Center (CHU) of Limoges, Limoges, FranceRelationships between c-Rel and GCB-DLBCLs remain unclear. We found that strong c-Rel DNA-binding activity was mostly found in GCBs on two independent series of 48 DLBCLs and 66 DLBCLs, the latter issued from the GHEDI series. c-Rel DNA-binding activity was associated with increased REL mRNA expression. Extending the study to the whole GHEDI and Lenz DLBCL published series of 202 and 233 cases, it was found that the c-Rel gene expression profile (GEP) overlapped partially (12%) but only with the GCB GEP and not with the GEP of ABC-DLBCLs. Cases with both overexpression of REL mRNA and c-Rel GEP were defined as those having a c-Rel signature. These cases were GCBs in 88 and 83% of the GHEDI or Lenz’s DLBCL series respectively. The c-Rel signature was also associated with various recurrent GCB-DLBCL genetic events, including REL gains, BCL2 translocation, MEF2B, EZH2, CREBBP, and TNFRSF14 mutations and with the EZB GCB genetic subtype. By CGH array, the c-Rel signature was specifically correlated with 2p15-16.1 amplification that includes XPO1, BCL11A, and USP34 and with the 22q11.22 deletion that covers IGLL5 and PRAME. The total number of gene copy number aberrations, so-called genomic imbalance complexity, was decreased in cases with the c-Rel signature. These cases exhibited a better overall survival. Functionally, overexpression of c-Rel induced its constitutive nuclear localization and protected cells against apoptosis while its repression tended to increase cell death. These results show that, clinically and biologically, c-Rel is the pivotal NF-κB subunit in the GCB-DLBCL subgroup. Functionally, c-Rel overexpression could directly promote DLBCL tumorigenesis without need for further activation signals.https://www.frontiersin.org/articles/10.3389/fonc.2021.638897/fullNF-kappaBDNA binding activityc-Relgerminal center B-cell–diffuse large B-cell lymphomagenetic alterations

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