Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency

Background. AT/RTs are rare aggressive brain tumours, mainly affecting young children. Most cases present with genetic inactivation of SMARCB1, a core member of the SWI/SNF chromatin-remodeling complex. We have performed whole exome- and mRNA-sequencing on an early onset AT/RT case for detection of...

Descripción completa

Detalles Bibliográficos
Autores principales: Sandgren, Johanna, Holm, Stefan, Marino, Ana Maria, Asmundsson, Jurate, Grillner, Pernilla, Nistér, Monica, Díaz de Ståhl, Teresita
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi Publishing Corporation 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4780067/
https://www.ncbi.nlm.nih.gov/pubmed/26998479
http://dx.doi.org/10.1155/2015/862039
_version_ 1782419707526119424
author Sandgren, Johanna
Holm, Stefan
Marino, Ana Maria
Asmundsson, Jurate
Grillner, Pernilla
Nistér, Monica
Díaz de Ståhl, Teresita
author_facet Sandgren, Johanna
Holm, Stefan
Marino, Ana Maria
Asmundsson, Jurate
Grillner, Pernilla
Nistér, Monica
Díaz de Ståhl, Teresita
author_sort Sandgren, Johanna
collection PubMed
description Background. AT/RTs are rare aggressive brain tumours, mainly affecting young children. Most cases present with genetic inactivation of SMARCB1, a core member of the SWI/SNF chromatin-remodeling complex. We have performed whole exome- and mRNA-sequencing on an early onset AT/RT case for detection of genetic events potentially contributing to the disease. Results. A de novo germline variant in SMARCB1, c.601C>T p.Arg201(∗), in combination with somatic deletion of the healthy allele is likely the major tumour causing event. Only seven somatic small scale mutations were discovered (hitting SEPT03, H2BFM, ZIC4, HIST2H2AB, ZIK1, KRTAP6-3, and IFNA8). All were found with subclonal allele frequencies (range 5.7–17%) and none were expressed. However, besides SMARCB1, candidate genes affected by predicted damaging germline variants that were expressed were detected (KDM5C, NUMA1, and PCM1). Analysis of differently expressed genes revealed many dysregulated pathways in the tumour, such as cell cycle, CXCR4 pathway, GPCR-signalling, and neuronal system. FGFR1, CXCR4, and MDK were upregulated and may represent possible drug targets. Conclusion. The loss of SMARCB1 function leads to AT/RT development and deregulated genes and pathways. Additional predisposing events may however contribute. Studies utilizing NGS technologies in larger cohorts will probably identify recurrent genetic and epigenetic alterations and molecular subgroups with implications for clinical practice and development of targeted therapies.
format Online
Article
Text
id pubmed-4780067
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Hindawi Publishing Corporation
record_format MEDLINE/PubMed
spelling pubmed-47800672016-03-20 Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency Sandgren, Johanna Holm, Stefan Marino, Ana Maria Asmundsson, Jurate Grillner, Pernilla Nistér, Monica Díaz de Ståhl, Teresita Biomed Res Int Research Article Background. AT/RTs are rare aggressive brain tumours, mainly affecting young children. Most cases present with genetic inactivation of SMARCB1, a core member of the SWI/SNF chromatin-remodeling complex. We have performed whole exome- and mRNA-sequencing on an early onset AT/RT case for detection of genetic events potentially contributing to the disease. Results. A de novo germline variant in SMARCB1, c.601C>T p.Arg201(∗), in combination with somatic deletion of the healthy allele is likely the major tumour causing event. Only seven somatic small scale mutations were discovered (hitting SEPT03, H2BFM, ZIC4, HIST2H2AB, ZIK1, KRTAP6-3, and IFNA8). All were found with subclonal allele frequencies (range 5.7–17%) and none were expressed. However, besides SMARCB1, candidate genes affected by predicted damaging germline variants that were expressed were detected (KDM5C, NUMA1, and PCM1). Analysis of differently expressed genes revealed many dysregulated pathways in the tumour, such as cell cycle, CXCR4 pathway, GPCR-signalling, and neuronal system. FGFR1, CXCR4, and MDK were upregulated and may represent possible drug targets. Conclusion. The loss of SMARCB1 function leads to AT/RT development and deregulated genes and pathways. Additional predisposing events may however contribute. Studies utilizing NGS technologies in larger cohorts will probably identify recurrent genetic and epigenetic alterations and molecular subgroups with implications for clinical practice and development of targeted therapies. Hindawi Publishing Corporation 2015 2015-08-12 /pmc/articles/PMC4780067/ /pubmed/26998479 http://dx.doi.org/10.1155/2015/862039 Text en Copyright © 2015 Johanna Sandgren et al. https://creativecommons.org/licenses/by/3.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Sandgren, Johanna
Holm, Stefan
Marino, Ana Maria
Asmundsson, Jurate
Grillner, Pernilla
Nistér, Monica
Díaz de Ståhl, Teresita
Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency
title Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency
title_full Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency
title_fullStr Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency
title_full_unstemmed Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency
title_short Whole Exome- and mRNA-Sequencing of an AT/RT Case Reveals Few Somatic Mutations and Several Deregulated Signalling Pathways in the Context of SMARCB1 Deficiency
title_sort whole exome- and mrna-sequencing of an at/rt case reveals few somatic mutations and several deregulated signalling pathways in the context of smarcb1 deficiency
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4780067/
https://www.ncbi.nlm.nih.gov/pubmed/26998479
http://dx.doi.org/10.1155/2015/862039
work_keys_str_mv AT sandgrenjohanna wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency
AT holmstefan wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency
AT marinoanamaria wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency
AT asmundssonjurate wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency
AT grillnerpernilla wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency
AT nistermonica wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency
AT diazdestahlteresita wholeexomeandmrnasequencingofanatrtcaserevealsfewsomaticmutationsandseveralderegulatedsignallingpathwaysinthecontextofsmarcb1deficiency

Ejemplares similares