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Functional significance of germline EPAS1 variants

Mosaic or somatic EPAS1 mutations are associated with a range of phenotypes including pheochromocytoma and/or paraganglioma (PPGL), polycythemia and somatostatinoma. The pathogenic potential of germline EPAS1 variants however is not well understood. We report a number of germline EPAS1 variants occu...

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Autores principales: Dwight, Trisha, Kim, Edward, Bastard, Karine, Benn, Diana E, Eisenhofer, Graeme, Richter, Susan, Mannelli, Massimo, Rapizzi, Elena, Prejbisz, Aleksander, Pęczkowska, Mariola, Pacak, Karel, Clifton-Bligh, Roderick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Bioscientifica Ltd 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7989857/
https://www.ncbi.nlm.nih.gov/pubmed/33300499
http://dx.doi.org/10.1530/ERC-20-0280
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author Dwight, Trisha
Kim, Edward
Bastard, Karine
Benn, Diana E
Eisenhofer, Graeme
Richter, Susan
Mannelli, Massimo
Rapizzi, Elena
Prejbisz, Aleksander
Pęczkowska, Mariola
Pacak, Karel
Clifton-Bligh, Roderick
author_facet Dwight, Trisha
Kim, Edward
Bastard, Karine
Benn, Diana E
Eisenhofer, Graeme
Richter, Susan
Mannelli, Massimo
Rapizzi, Elena
Prejbisz, Aleksander
Pęczkowska, Mariola
Pacak, Karel
Clifton-Bligh, Roderick
author_sort Dwight, Trisha
collection PubMed
description Mosaic or somatic EPAS1 mutations are associated with a range of phenotypes including pheochromocytoma and/or paraganglioma (PPGL), polycythemia and somatostatinoma. The pathogenic potential of germline EPAS1 variants however is not well understood. We report a number of germline EPAS1 variants occurring in patients with PPGL, including a novel variant c.739C>A (p.Arg247Ser); a previously described variant c.1121T>A (p.Phe374Tyr); several rare variants, c.581A>G (p.His194Arg), c.2353C>A (p.Pro785Thr) and c.2365A>G (p.Ile789Val); a common variant c.2296A>C (p.Thr766Pro). We performed detailed functional studies to understand their pathogenic role in PPGL. In transient transfection studies, EPAS1/HIF-2α p.Arg247Ser, p.Phe374Tyr and p.Pro785Thr were all stable in normoxia. In co-immunoprecipitation assays, only the novel variant p.Arg247Ser showed diminished interaction with pVHL. A direct interaction between HIF-2α Arg247 and pVHL was confirmed in structural models. Transactivation was assessed by means of a HRE-containing reporter gene in transiently transfected cells, and significantly higher reporter activity was only observed with EPAS1/HIF-2α p.Phe374Tyr and p.Pro785Thr. In conclusion, three germline EPAS1 variants (c.739C>A (p.Arg247Ser), c.1121T>A (p.Phe374Tyr) and c.2353C>A (p.Pro785Thr)) all have some functional features in common with somatic activating mutations. Our findings suggest that these three germline variants are hypermorphic alleles that may act as modifiers to the expression of PPGLs.
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spelling pubmed-79898572021-03-31 Functional significance of germline EPAS1 variants Dwight, Trisha Kim, Edward Bastard, Karine Benn, Diana E Eisenhofer, Graeme Richter, Susan Mannelli, Massimo Rapizzi, Elena Prejbisz, Aleksander Pęczkowska, Mariola Pacak, Karel Clifton-Bligh, Roderick Endocr Relat Cancer Research Mosaic or somatic EPAS1 mutations are associated with a range of phenotypes including pheochromocytoma and/or paraganglioma (PPGL), polycythemia and somatostatinoma. The pathogenic potential of germline EPAS1 variants however is not well understood. We report a number of germline EPAS1 variants occurring in patients with PPGL, including a novel variant c.739C>A (p.Arg247Ser); a previously described variant c.1121T>A (p.Phe374Tyr); several rare variants, c.581A>G (p.His194Arg), c.2353C>A (p.Pro785Thr) and c.2365A>G (p.Ile789Val); a common variant c.2296A>C (p.Thr766Pro). We performed detailed functional studies to understand their pathogenic role in PPGL. In transient transfection studies, EPAS1/HIF-2α p.Arg247Ser, p.Phe374Tyr and p.Pro785Thr were all stable in normoxia. In co-immunoprecipitation assays, only the novel variant p.Arg247Ser showed diminished interaction with pVHL. A direct interaction between HIF-2α Arg247 and pVHL was confirmed in structural models. Transactivation was assessed by means of a HRE-containing reporter gene in transiently transfected cells, and significantly higher reporter activity was only observed with EPAS1/HIF-2α p.Phe374Tyr and p.Pro785Thr. In conclusion, three germline EPAS1 variants (c.739C>A (p.Arg247Ser), c.1121T>A (p.Phe374Tyr) and c.2353C>A (p.Pro785Thr)) all have some functional features in common with somatic activating mutations. Our findings suggest that these three germline variants are hypermorphic alleles that may act as modifiers to the expression of PPGLs. Bioscientifica Ltd 2020-12-07 /pmc/articles/PMC7989857/ /pubmed/33300499 http://dx.doi.org/10.1530/ERC-20-0280 Text en © 2021 The authors http://creativecommons.org/licenses/by/4.0/ This work is licensed under a Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research
Dwight, Trisha
Kim, Edward
Bastard, Karine
Benn, Diana E
Eisenhofer, Graeme
Richter, Susan
Mannelli, Massimo
Rapizzi, Elena
Prejbisz, Aleksander
Pęczkowska, Mariola
Pacak, Karel
Clifton-Bligh, Roderick
Functional significance of germline EPAS1 variants
title Functional significance of germline EPAS1 variants
title_full Functional significance of germline EPAS1 variants
title_fullStr Functional significance of germline EPAS1 variants
title_full_unstemmed Functional significance of germline EPAS1 variants
title_short Functional significance of germline EPAS1 variants
title_sort functional significance of germline epas1 variants
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7989857/
https://www.ncbi.nlm.nih.gov/pubmed/33300499
http://dx.doi.org/10.1530/ERC-20-0280
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