β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression

Desmoid‐type fibromatosis (DF) is a rare mesenchymal lesion with high risk of local recurrence. Specific β‐catenin mutations (S45F) appeared to be related to this higher risk compared to T41A‐mutated or wild‐type (WT). We explored the influence of both mutations and WT on structure stability and aff...

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Autores principales: Colombo, Chiara, Belfiore, Antonino, Paielli, Nicholas, De Cecco, Loris, Canevari, Silvana, Laurini, Erik, Fermeglia, Maurizio, Pricl, Sabrina, Verderio, Paolo, Bottelli, Stefano, Fiore, Marco, Stacchiotti, Silvia, Palassini, Elena, Gronchi, Alessandro, Pilotti, Silvana, Perrone, Federica
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5664003/
https://www.ncbi.nlm.nih.gov/pubmed/28627792
http://dx.doi.org/10.1002/1878-0261.12101
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author Colombo, Chiara
Belfiore, Antonino
Paielli, Nicholas
De Cecco, Loris
Canevari, Silvana
Laurini, Erik
Fermeglia, Maurizio
Pricl, Sabrina
Verderio, Paolo
Bottelli, Stefano
Fiore, Marco
Stacchiotti, Silvia
Palassini, Elena
Gronchi, Alessandro
Pilotti, Silvana
Perrone, Federica
author_facet Colombo, Chiara
Belfiore, Antonino
Paielli, Nicholas
De Cecco, Loris
Canevari, Silvana
Laurini, Erik
Fermeglia, Maurizio
Pricl, Sabrina
Verderio, Paolo
Bottelli, Stefano
Fiore, Marco
Stacchiotti, Silvia
Palassini, Elena
Gronchi, Alessandro
Pilotti, Silvana
Perrone, Federica
author_sort Colombo, Chiara
collection PubMed
description Desmoid‐type fibromatosis (DF) is a rare mesenchymal lesion with high risk of local recurrence. Specific β‐catenin mutations (S45F) appeared to be related to this higher risk compared to T41A‐mutated or wild‐type (WT). We explored the influence of both mutations and WT on structure stability and affinity of β‐catenin for α‐catenin and the pattern of gene expression that may influence DF behavior. Using 33 surgically resected primary DFs harboring T41A (n = 14), S45F (n = 10), or WT (n = 9), we performed a comparative molecular analysis by protein/protein interaction modeling, gene expression by DASL microarrays, human inflammation gene panel, and assessment of immune system‐based biomarkers by immunohistochemistry. Mutated proteins were more stable than WT and formed a weaker complex with α‐catenin. Consensus unsupervised gene clustering revealed the presence of two DF group‐mutated (T41A + S45F) and WT (P = 0.0047). The gene sets ‘Inflammatory‐Defense‐Humoral Immune Response’ and ‘Antigen Binding’ were significantly enriched in T41A. The deregulation of 16 inflammation‐related genes was confirmed. Low numbers of T cells and tumor‐associated macrophages (TAM) infiltrating the tumors and low/absent PD‐1/PD‐L1 expression were also identified. We demonstrated that mutated DFs (T41A or S45F) and WT are two distinct molecular subgroups with regard to β‐catenin stability, α‐catenin affinity, and gene expression profiling. A different inflammation signature characterized the two mutated groups, suggesting mediation either by T41A or by S45F. Finally, all mutated cases showed a low number of TIL and TAM cells and a low or absent expression of PD‐1 and PD‐L1 consistent with β‐catenin activation insensitive to checkpoint blockade.
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spelling pubmed-56640032017-11-06 β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression Colombo, Chiara Belfiore, Antonino Paielli, Nicholas De Cecco, Loris Canevari, Silvana Laurini, Erik Fermeglia, Maurizio Pricl, Sabrina Verderio, Paolo Bottelli, Stefano Fiore, Marco Stacchiotti, Silvia Palassini, Elena Gronchi, Alessandro Pilotti, Silvana Perrone, Federica Mol Oncol Research Articles Desmoid‐type fibromatosis (DF) is a rare mesenchymal lesion with high risk of local recurrence. Specific β‐catenin mutations (S45F) appeared to be related to this higher risk compared to T41A‐mutated or wild‐type (WT). We explored the influence of both mutations and WT on structure stability and affinity of β‐catenin for α‐catenin and the pattern of gene expression that may influence DF behavior. Using 33 surgically resected primary DFs harboring T41A (n = 14), S45F (n = 10), or WT (n = 9), we performed a comparative molecular analysis by protein/protein interaction modeling, gene expression by DASL microarrays, human inflammation gene panel, and assessment of immune system‐based biomarkers by immunohistochemistry. Mutated proteins were more stable than WT and formed a weaker complex with α‐catenin. Consensus unsupervised gene clustering revealed the presence of two DF group‐mutated (T41A + S45F) and WT (P = 0.0047). The gene sets ‘Inflammatory‐Defense‐Humoral Immune Response’ and ‘Antigen Binding’ were significantly enriched in T41A. The deregulation of 16 inflammation‐related genes was confirmed. Low numbers of T cells and tumor‐associated macrophages (TAM) infiltrating the tumors and low/absent PD‐1/PD‐L1 expression were also identified. We demonstrated that mutated DFs (T41A or S45F) and WT are two distinct molecular subgroups with regard to β‐catenin stability, α‐catenin affinity, and gene expression profiling. A different inflammation signature characterized the two mutated groups, suggesting mediation either by T41A or by S45F. Finally, all mutated cases showed a low number of TIL and TAM cells and a low or absent expression of PD‐1 and PD‐L1 consistent with β‐catenin activation insensitive to checkpoint blockade. John Wiley and Sons Inc. 2017-09-29 2017-11 /pmc/articles/PMC5664003/ /pubmed/28627792 http://dx.doi.org/10.1002/1878-0261.12101 Text en © 2017 The Authors. Published by FEBS Press and John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Colombo, Chiara
Belfiore, Antonino
Paielli, Nicholas
De Cecco, Loris
Canevari, Silvana
Laurini, Erik
Fermeglia, Maurizio
Pricl, Sabrina
Verderio, Paolo
Bottelli, Stefano
Fiore, Marco
Stacchiotti, Silvia
Palassini, Elena
Gronchi, Alessandro
Pilotti, Silvana
Perrone, Federica
β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression
title β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression
title_full β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression
title_fullStr β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression
title_full_unstemmed β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression
title_short β‐Catenin in desmoid‐type fibromatosis: deep insights into the role of T41A and S45F mutations on protein structure and gene expression
title_sort β‐catenin in desmoid‐type fibromatosis: deep insights into the role of t41a and s45f mutations on protein structure and gene expression
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5664003/
https://www.ncbi.nlm.nih.gov/pubmed/28627792
http://dx.doi.org/10.1002/1878-0261.12101
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