MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome

APC is the key gene of the familial adenomatous polyposis (FAP). This tumor suppressor gene functions by negatively regulating the β-catenin protein and the majority of APC mutations disrupt the β-catenin degradation complex signalosome leading to the activation of the canonical Wnt pathway. Pathoge...

Descripción completa

Detalles Bibliográficos
Autores principales: Abdelmoula, Balkiss, Abid, Fatma, Karra, Amir, Kammoun, Sonda, Aloulou, Samir, Abdelmoula, Nouha Bouayed
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2022
Materias:
Medulloblastoma
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165304/
http://dx.doi.org/10.1093/neuonc/noac079.376
_version_ 1784720362231037952
author Abdelmoula, Balkiss
Abid, Fatma
Karra, Amir
Kammoun, Sonda
Aloulou, Samir
Abdelmoula, Nouha Bouayed
author_facet Abdelmoula, Balkiss
Abid, Fatma
Karra, Amir
Kammoun, Sonda
Aloulou, Samir
Abdelmoula, Nouha Bouayed
author_sort Abdelmoula, Balkiss
collection PubMed
description APC is the key gene of the familial adenomatous polyposis (FAP). This tumor suppressor gene functions by negatively regulating the β-catenin protein and the majority of APC mutations disrupt the β-catenin degradation complex signalosome leading to the activation of the canonical Wnt pathway. Pathogenic APC mutations were reported in association to medulloblastoma. In this study, we report rare mutations of the APC gene detected in Tunisian families from the governorate of Sfax presenting clinically with various digestive and extra-digestive manifestations. Our goal was to assess the oncogenic risks encountered by our pediatric carriers to offer an accurate genetic counselling, particularly at the neurologic level. Molecular investigation of all members of two families was conducted, using bidirectional sequencing of all 15 exons of the APC gene. A phenotype-genotype correlation was conducted to elucidate the mutational pathophysiological mechanism. Two rare mutations were revealed in our familial study. The first mutation was located at exon 13 and was a missense mutation at codon 1690. The second mutation was a deletion identified at codon 4652 in exon 15. The mutations resulted both in truncated gene products. Clinical manifestations closely depending on the position of the mutation were respectively colic polyposis for the first mutation and soft tissue fibromatous tumors for the second. The localization of the APC mutations allows better targeting of surveillance for clinical manifestations that may be included in FAP. Mutations that remove the Axin-binding sites, as is the case for the first mutation, lead to severe clinical pictures whereas mutations that retain one or two of the Axin binding sites are associated with other features such as desmoid tumors. The risk of the Wnt- medulloblastoma subtype, higher among patients with FAP should be considered with a more awareness of signs and symptoms related to CNS tumors in the FAP context.
format Online
Article
Text
id pubmed-9165304
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-91653042022-06-06 MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome Abdelmoula, Balkiss Abid, Fatma Karra, Amir Kammoun, Sonda Aloulou, Samir Abdelmoula, Nouha Bouayed Neuro Oncol Medulloblastoma APC is the key gene of the familial adenomatous polyposis (FAP). This tumor suppressor gene functions by negatively regulating the β-catenin protein and the majority of APC mutations disrupt the β-catenin degradation complex signalosome leading to the activation of the canonical Wnt pathway. Pathogenic APC mutations were reported in association to medulloblastoma. In this study, we report rare mutations of the APC gene detected in Tunisian families from the governorate of Sfax presenting clinically with various digestive and extra-digestive manifestations. Our goal was to assess the oncogenic risks encountered by our pediatric carriers to offer an accurate genetic counselling, particularly at the neurologic level. Molecular investigation of all members of two families was conducted, using bidirectional sequencing of all 15 exons of the APC gene. A phenotype-genotype correlation was conducted to elucidate the mutational pathophysiological mechanism. Two rare mutations were revealed in our familial study. The first mutation was located at exon 13 and was a missense mutation at codon 1690. The second mutation was a deletion identified at codon 4652 in exon 15. The mutations resulted both in truncated gene products. Clinical manifestations closely depending on the position of the mutation were respectively colic polyposis for the first mutation and soft tissue fibromatous tumors for the second. The localization of the APC mutations allows better targeting of surveillance for clinical manifestations that may be included in FAP. Mutations that remove the Axin-binding sites, as is the case for the first mutation, lead to severe clinical pictures whereas mutations that retain one or two of the Axin binding sites are associated with other features such as desmoid tumors. The risk of the Wnt- medulloblastoma subtype, higher among patients with FAP should be considered with a more awareness of signs and symptoms related to CNS tumors in the FAP context. Oxford University Press 2022-06-03 /pmc/articles/PMC9165304/ http://dx.doi.org/10.1093/neuonc/noac079.376 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 Medulloblastoma
Abdelmoula, Balkiss
Abid, Fatma
Karra, Amir
Kammoun, Sonda
Aloulou, Samir
Abdelmoula, Nouha Bouayed
MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome
title MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome
title_full MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome
title_fullStr MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome
title_full_unstemmed MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome
title_short MEDB-01. Management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated Wnt signalosome
title_sort medb-01. management of the risk of medulloblastoma associated to familial adenomatous polyposis and dysregulated wnt signalosome
topic Medulloblastoma
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9165304/
http://dx.doi.org/10.1093/neuonc/noac079.376
work_keys_str_mv AT abdelmoulabalkiss medb01managementoftheriskofmedulloblastomaassociatedtofamilialadenomatouspolyposisanddysregulatedwntsignalosome
AT abidfatma medb01managementoftheriskofmedulloblastomaassociatedtofamilialadenomatouspolyposisanddysregulatedwntsignalosome
AT karraamir medb01managementoftheriskofmedulloblastomaassociatedtofamilialadenomatouspolyposisanddysregulatedwntsignalosome
AT kammounsonda medb01managementoftheriskofmedulloblastomaassociatedtofamilialadenomatouspolyposisanddysregulatedwntsignalosome
AT aloulousamir medb01managementoftheriskofmedulloblastomaassociatedtofamilialadenomatouspolyposisanddysregulatedwntsignalosome
AT abdelmoulanouhabouayed medb01managementoftheriskofmedulloblastomaassociatedtofamilialadenomatouspolyposisanddysregulatedwntsignalosome

Ejemplares similares