Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis

SIMPLE SUMMARY: Diffuse grade II IDH-mutant gliomas are rare brain tumors mainly affecting young patients. These tumors are composed of different populations of tumoral cells. Little is known of these cells and how they are generated. These different cells may show different sensitivity to treatment...

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Autores principales: Augustus, Meera, Pineau, Donovan, Aimond, Franck, Azar, Safa, Lecca, Davide, Scamps, Frédérique, Muxel, Sophie, Darlix, Amélie, Ritchie, William, Gozé, Catherine, Rigau, Valérie, Duffau, Hugues, Hugnot, Jean-Philippe
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8123787/
https://www.ncbi.nlm.nih.gov/pubmed/33925547
http://dx.doi.org/10.3390/cancers13092107
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author Augustus, Meera
Pineau, Donovan
Aimond, Franck
Azar, Safa
Lecca, Davide
Scamps, Frédérique
Muxel, Sophie
Darlix, Amélie
Ritchie, William
Gozé, Catherine
Rigau, Valérie
Duffau, Hugues
Hugnot, Jean-Philippe
author_facet Augustus, Meera
Pineau, Donovan
Aimond, Franck
Azar, Safa
Lecca, Davide
Scamps, Frédérique
Muxel, Sophie
Darlix, Amélie
Ritchie, William
Gozé, Catherine
Rigau, Valérie
Duffau, Hugues
Hugnot, Jean-Philippe
author_sort Augustus, Meera
collection PubMed
description SIMPLE SUMMARY: Diffuse grade II IDH-mutant gliomas are rare brain tumors mainly affecting young patients. These tumors are composed of different populations of tumoral cells. Little is known of these cells and how they are generated. These different cells may show different sensitivity to treatments, so our aim was to study them in detail by directly using patient resections. We identified two clearly distinct tumoral populations and defined reliable markers for them. We also uncovered part of the molecular mechanisms that generate them. Finally, we found that the two cell types have different electrical activity. This article provides unique data and new issues on these rare tumors, which need to be further investigated to develop innovative treatments. ABSTRACT: Diffuse grade II IDH-mutant gliomas are slow-growing brain tumors that progress into high-grade gliomas. They present intratumoral cell heterogeneity, and no reliable markers are available to distinguish the different cell subtypes. The molecular mechanisms underlying the formation of this cell diversity is also ill-defined. Here, we report that SOX9 and OLIG1 transcription factors, which specifically label astrocytes and oligodendrocytes in the normal brain, revealed the presence of two largely nonoverlapping tumoral populations in IDH1-mutant oligodendrogliomas and astrocytomas. Astrocyte-like SOX9(+) cells additionally stained for APOE, CRYAB, ID4, KCNN3, while oligodendrocyte-like OLIG1(+) cells stained for ASCL1, EGFR, IDH1, PDGFRA, PTPRZ1, SOX4, and SOX8. GPR17, an oligodendrocytic marker, was expressed by both cells. These two subpopulations appear to have distinct BMP, NOTCH1, and MAPK active pathways as stainings for BMP4, HEY1, HEY2, p-SMAD1/5 and p-ERK were higher in SOX9(+) cells. We used primary cultures and a new cell line to explore the influence of NOTCH1 activation and BMP treatment on the IDH1-mutant glioma cell phenotype. This revealed that NOTCH1 globally reduced oligodendrocytic markers and IDH1 expression while upregulating APOE, CRYAB, HEY1/2, and an electrophysiologically-active Ca(2+)-activated apamin-sensitive K(+) channel (KCNN3/SK3). This was accompanied by a reduction in proliferation. Similar effects of NOTCH1 activation were observed in nontumoral human oligodendrocytic cells, which additionally induced strong SOX9 expression. BMP treatment reduced OLIG1/2 expression and strongly upregulated CRYAB and NOGGIN, a negative regulator of BMP. The presence of astrocyte-like SOX9(+) and oligodendrocyte-like OLIG1(+) cells in grade II IDH1-mutant gliomas raises new questions about their role in the pathology.
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spelling pubmed-81237872021-05-16 Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis Augustus, Meera Pineau, Donovan Aimond, Franck Azar, Safa Lecca, Davide Scamps, Frédérique Muxel, Sophie Darlix, Amélie Ritchie, William Gozé, Catherine Rigau, Valérie Duffau, Hugues Hugnot, Jean-Philippe Cancers (Basel) Article SIMPLE SUMMARY: Diffuse grade II IDH-mutant gliomas are rare brain tumors mainly affecting young patients. These tumors are composed of different populations of tumoral cells. Little is known of these cells and how they are generated. These different cells may show different sensitivity to treatments, so our aim was to study them in detail by directly using patient resections. We identified two clearly distinct tumoral populations and defined reliable markers for them. We also uncovered part of the molecular mechanisms that generate them. Finally, we found that the two cell types have different electrical activity. This article provides unique data and new issues on these rare tumors, which need to be further investigated to develop innovative treatments. ABSTRACT: Diffuse grade II IDH-mutant gliomas are slow-growing brain tumors that progress into high-grade gliomas. They present intratumoral cell heterogeneity, and no reliable markers are available to distinguish the different cell subtypes. The molecular mechanisms underlying the formation of this cell diversity is also ill-defined. Here, we report that SOX9 and OLIG1 transcription factors, which specifically label astrocytes and oligodendrocytes in the normal brain, revealed the presence of two largely nonoverlapping tumoral populations in IDH1-mutant oligodendrogliomas and astrocytomas. Astrocyte-like SOX9(+) cells additionally stained for APOE, CRYAB, ID4, KCNN3, while oligodendrocyte-like OLIG1(+) cells stained for ASCL1, EGFR, IDH1, PDGFRA, PTPRZ1, SOX4, and SOX8. GPR17, an oligodendrocytic marker, was expressed by both cells. These two subpopulations appear to have distinct BMP, NOTCH1, and MAPK active pathways as stainings for BMP4, HEY1, HEY2, p-SMAD1/5 and p-ERK were higher in SOX9(+) cells. We used primary cultures and a new cell line to explore the influence of NOTCH1 activation and BMP treatment on the IDH1-mutant glioma cell phenotype. This revealed that NOTCH1 globally reduced oligodendrocytic markers and IDH1 expression while upregulating APOE, CRYAB, HEY1/2, and an electrophysiologically-active Ca(2+)-activated apamin-sensitive K(+) channel (KCNN3/SK3). This was accompanied by a reduction in proliferation. Similar effects of NOTCH1 activation were observed in nontumoral human oligodendrocytic cells, which additionally induced strong SOX9 expression. BMP treatment reduced OLIG1/2 expression and strongly upregulated CRYAB and NOGGIN, a negative regulator of BMP. The presence of astrocyte-like SOX9(+) and oligodendrocyte-like OLIG1(+) cells in grade II IDH1-mutant gliomas raises new questions about their role in the pathology. MDPI 2021-04-27 /pmc/articles/PMC8123787/ /pubmed/33925547 http://dx.doi.org/10.3390/cancers13092107 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Augustus, Meera
Pineau, Donovan
Aimond, Franck
Azar, Safa
Lecca, Davide
Scamps, Frédérique
Muxel, Sophie
Darlix, Amélie
Ritchie, William
Gozé, Catherine
Rigau, Valérie
Duffau, Hugues
Hugnot, Jean-Philippe
Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis
title Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis
title_full Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis
title_fullStr Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis
title_full_unstemmed Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis
title_short Identification of CRYAB(+) KCNN3(+) SOX9(+) Astrocyte-Like and EGFR(+) PDGFRA(+) OLIG1(+) Oligodendrocyte-Like Tumoral Cells in Diffuse IDH1-Mutant Gliomas and Implication of NOTCH1 Signalling in Their Genesis
title_sort identification of cryab(+) kcnn3(+) sox9(+) astrocyte-like and egfr(+) pdgfra(+) olig1(+) oligodendrocyte-like tumoral cells in diffuse idh1-mutant gliomas and implication of notch1 signalling in their genesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8123787/
https://www.ncbi.nlm.nih.gov/pubmed/33925547
http://dx.doi.org/10.3390/cancers13092107
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