RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours

Craniopharyngiomas are rare challenging tumours, with around 25% of cases recurring despite surgery and/or radiotherapy. Whilst transcriptomic and proteomic profiling of adamantinomatous craniopharyngioma (ACP) have revealed activation of the MAPK pathway and IL-6 mediated inflammation, relatively l...

Descripción completa

Detalles Bibliográficos
Autores principales: Apps, John, Pickles, Jessica, Stone, Thomas, Chalker, Jane, Ogunbiyi, Olumide, Schwalbe, Edward, Brandner, Sebastian, Otto, Georg, Castellano, Sergi, Jacques, Thomas, Deutschbein, Timo, Martinez-Barbera, Juan Pedro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Craniopharyngioma and Rare Tumors
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165309/
http://dx.doi.org/10.1093/neuonc/noac079.033
_version_ 1784720363505057792
author Apps, John
Pickles, Jessica
Stone, Thomas
Chalker, Jane
Ogunbiyi, Olumide
Schwalbe, Edward
Brandner, Sebastian
Otto, Georg
Castellano, Sergi
Jacques, Thomas
Deutschbein, Timo
Martinez-Barbera, Juan Pedro
author_facet Apps, John
Pickles, Jessica
Stone, Thomas
Chalker, Jane
Ogunbiyi, Olumide
Schwalbe, Edward
Brandner, Sebastian
Otto, Georg
Castellano, Sergi
Jacques, Thomas
Deutschbein, Timo
Martinez-Barbera, Juan Pedro
author_sort Apps, John
collection PubMed
description Craniopharyngiomas are rare challenging tumours, with around 25% of cases recurring despite surgery and/or radiotherapy. Whilst transcriptomic and proteomic profiling of adamantinomatous craniopharyngioma (ACP) have revealed activation of the MAPK pathway and IL-6 mediated inflammation, relatively little is known about the biological processes involved in tumour recurrence. To address this, we have analysed a cohort of primary and relapsed ACP tumour accessed from tissue banks, local pathology departments and international collaborators. Serial samples of recurrent ACP (n=11), recurrent papillary craniopharyngioma (PCP) (n=4) and 3 non-recurrent ACP were analysed using β-catenin, pERK1/2 immunostaining, DNA methylation array and RNA sequencing. Differential expression and methylation analyses confirmed differences between ACP and PCP, with over representation of WNT pathway genes in ACP and the MAPK pathway genes in PCP. All of the primary and all except for one of the relapsed ACP tumours showed a pERK1/2 expression. Differences in the immune environment were also identified between ACP and PCP, with higher levels of some inflammatory mediators and CD14+ cell signatures in PCP compared with ACP. Whilst differential methylation and expression analysis revealed relatively stable methylomes and transcriptomes between serial samples of cases, segmental chromosomal alterations were identified in recurrence samples from five ACP cases (5/11,45%). One relapsed case showed histological and molecular signs of malignant transformation, including high ki67 and deletion of TP53. Surprisingly, this malignant tumour showed nuclear beta-catenin in all neoplastic epithelial cells and absence of pERK1/2 staining, despite the primary tumour showing the typical beta-catenin and pERK1/2 expression patterns. These results suggest that the molecular landscape of craniopharyngioma remains stable between recurrences in most cases, but, there is evidence of molecular evolution in a subset of cases. Activation of the MAPK pathway in the vast majority of ACP tumours supports the clinical evaluation of MAPK pathway inhibitors in ACP patients.
format Online
Article
Text
id pubmed-9165309
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-91653092022-06-06 RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours Apps, John Pickles, Jessica Stone, Thomas Chalker, Jane Ogunbiyi, Olumide Schwalbe, Edward Brandner, Sebastian Otto, Georg Castellano, Sergi Jacques, Thomas Deutschbein, Timo Martinez-Barbera, Juan Pedro Neuro Oncol Craniopharyngioma and Rare Tumors Craniopharyngiomas are rare challenging tumours, with around 25% of cases recurring despite surgery and/or radiotherapy. Whilst transcriptomic and proteomic profiling of adamantinomatous craniopharyngioma (ACP) have revealed activation of the MAPK pathway and IL-6 mediated inflammation, relatively little is known about the biological processes involved in tumour recurrence. To address this, we have analysed a cohort of primary and relapsed ACP tumour accessed from tissue banks, local pathology departments and international collaborators. Serial samples of recurrent ACP (n=11), recurrent papillary craniopharyngioma (PCP) (n=4) and 3 non-recurrent ACP were analysed using β-catenin, pERK1/2 immunostaining, DNA methylation array and RNA sequencing. Differential expression and methylation analyses confirmed differences between ACP and PCP, with over representation of WNT pathway genes in ACP and the MAPK pathway genes in PCP. All of the primary and all except for one of the relapsed ACP tumours showed a pERK1/2 expression. Differences in the immune environment were also identified between ACP and PCP, with higher levels of some inflammatory mediators and CD14+ cell signatures in PCP compared with ACP. Whilst differential methylation and expression analysis revealed relatively stable methylomes and transcriptomes between serial samples of cases, segmental chromosomal alterations were identified in recurrence samples from five ACP cases (5/11,45%). One relapsed case showed histological and molecular signs of malignant transformation, including high ki67 and deletion of TP53. Surprisingly, this malignant tumour showed nuclear beta-catenin in all neoplastic epithelial cells and absence of pERK1/2 staining, despite the primary tumour showing the typical beta-catenin and pERK1/2 expression patterns. These results suggest that the molecular landscape of craniopharyngioma remains stable between recurrences in most cases, but, there is evidence of molecular evolution in a subset of cases. Activation of the MAPK pathway in the vast majority of ACP tumours supports the clinical evaluation of MAPK pathway inhibitors in ACP patients. Oxford University Press 2022-06-03 /pmc/articles/PMC9165309/ http://dx.doi.org/10.1093/neuonc/noac079.033 Text en © The Author(s) 2022. Published by Oxford University Press on behalf of the Society for Neuro-Oncology. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Craniopharyngioma and Rare Tumors
Apps, John
Pickles, Jessica
Stone, Thomas
Chalker, Jane
Ogunbiyi, Olumide
Schwalbe, Edward
Brandner, Sebastian
Otto, Georg
Castellano, Sergi
Jacques, Thomas
Deutschbein, Timo
Martinez-Barbera, Juan Pedro
RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours
title RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours
title_full RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours
title_fullStr RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours
title_full_unstemmed RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours
title_short RARE-08. Profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the MAPK pathway and identifies copy number aberrations in relapsed tumours
title_sort rare-08. profiling of recurrent adamantinomatous cranionpharyngioma confirms the activation of the mapk pathway and identifies copy number aberrations in relapsed tumours
topic Craniopharyngioma and Rare Tumors
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165309/
http://dx.doi.org/10.1093/neuonc/noac079.033
work_keys_str_mv AT appsjohn rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT picklesjessica rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT stonethomas rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT chalkerjane rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT ogunbiyiolumide rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT schwalbeedward rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT brandnersebastian rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT ottogeorg rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT castellanosergi rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT jacquesthomas rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT deutschbeintimo rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours
AT martinezbarberajuanpedro rare08profilingofrecurrentadamantinomatouscranionpharyngiomaconfirmstheactivationofthemapkpathwayandidentifiescopynumberaberrationsinrelapsedtumours

Ejemplares similares