YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA

Medulloblastomas arise from undifferentiated precursor cells in the cerebellum and account for about 20% of all solid brain tumors during childhood; standard therapies include radiation and chemotherapy, which oftentimes come with severe impairment of the cognitive development of the young patients....

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Autores principales: Kloetgen, Andreas, Duggimpudi, Sujitha, Schuschel, Konstantin, Hezaveh, Kebria, Picard, Daniel, Schaal, Heiner, Remke, Marc, Klusmann, Jan-Henning, Borkhardt, Arndt, McHardy, Alice C., Hoell, Jessica I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7352269/
https://www.ncbi.nlm.nih.gov/pubmed/32585856
http://dx.doi.org/10.3390/ijms21124453
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author Kloetgen, Andreas
Duggimpudi, Sujitha
Schuschel, Konstantin
Hezaveh, Kebria
Picard, Daniel
Schaal, Heiner
Remke, Marc
Klusmann, Jan-Henning
Borkhardt, Arndt
McHardy, Alice C.
Hoell, Jessica I.
author_facet Kloetgen, Andreas
Duggimpudi, Sujitha
Schuschel, Konstantin
Hezaveh, Kebria
Picard, Daniel
Schaal, Heiner
Remke, Marc
Klusmann, Jan-Henning
Borkhardt, Arndt
McHardy, Alice C.
Hoell, Jessica I.
author_sort Kloetgen, Andreas
collection PubMed
description Medulloblastomas arise from undifferentiated precursor cells in the cerebellum and account for about 20% of all solid brain tumors during childhood; standard therapies include radiation and chemotherapy, which oftentimes come with severe impairment of the cognitive development of the young patients. Here, we show that the posttranscriptional regulator Y-box binding protein 1 (YBX1), a DNA- and RNA-binding protein, acts as an oncogene in medulloblastomas by regulating cellular survival and apoptosis. We observed different cellular responses upon YBX1 knockdown in several medulloblastoma cell lines, with significantly altered transcription and subsequent apoptosis rates. Mechanistically, PAR-CLIP for YBX1 and integration with RNA-Seq data uncovered direct posttranscriptional control of the heterochromatin-associated gene CBX5; upon YBX1 knockdown and subsequent CBX5 mRNA instability, heterochromatin-regulated genes involved in inflammatory response, apoptosis and death receptor signaling were de-repressed. Thus, YBX1 acts as an oncogene in medulloblastoma through indirect transcriptional regulation of inflammatory genes regulating apoptosis and represents a promising novel therapeutic target in this tumor entity.
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spelling pubmed-73522692020-07-21 YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA Kloetgen, Andreas Duggimpudi, Sujitha Schuschel, Konstantin Hezaveh, Kebria Picard, Daniel Schaal, Heiner Remke, Marc Klusmann, Jan-Henning Borkhardt, Arndt McHardy, Alice C. Hoell, Jessica I. Int J Mol Sci Article Medulloblastomas arise from undifferentiated precursor cells in the cerebellum and account for about 20% of all solid brain tumors during childhood; standard therapies include radiation and chemotherapy, which oftentimes come with severe impairment of the cognitive development of the young patients. Here, we show that the posttranscriptional regulator Y-box binding protein 1 (YBX1), a DNA- and RNA-binding protein, acts as an oncogene in medulloblastomas by regulating cellular survival and apoptosis. We observed different cellular responses upon YBX1 knockdown in several medulloblastoma cell lines, with significantly altered transcription and subsequent apoptosis rates. Mechanistically, PAR-CLIP for YBX1 and integration with RNA-Seq data uncovered direct posttranscriptional control of the heterochromatin-associated gene CBX5; upon YBX1 knockdown and subsequent CBX5 mRNA instability, heterochromatin-regulated genes involved in inflammatory response, apoptosis and death receptor signaling were de-repressed. Thus, YBX1 acts as an oncogene in medulloblastoma through indirect transcriptional regulation of inflammatory genes regulating apoptosis and represents a promising novel therapeutic target in this tumor entity. MDPI 2020-06-23 /pmc/articles/PMC7352269/ /pubmed/32585856 http://dx.doi.org/10.3390/ijms21124453 Text en © 2020 by the authors. 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 (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Kloetgen, Andreas
Duggimpudi, Sujitha
Schuschel, Konstantin
Hezaveh, Kebria
Picard, Daniel
Schaal, Heiner
Remke, Marc
Klusmann, Jan-Henning
Borkhardt, Arndt
McHardy, Alice C.
Hoell, Jessica I.
YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA
title YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA
title_full YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA
title_fullStr YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA
title_full_unstemmed YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA
title_short YBX1 Indirectly Targets Heterochromatin-Repressed Inflammatory Response-Related Apoptosis Genes through Regulating CBX5 mRNA
title_sort ybx1 indirectly targets heterochromatin-repressed inflammatory response-related apoptosis genes through regulating cbx5 mrna
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7352269/
https://www.ncbi.nlm.nih.gov/pubmed/32585856
http://dx.doi.org/10.3390/ijms21124453
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