Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome

The p63 gene encodes a master regulator of epidermal commitment, development, and differentiation. Heterozygous mutations in the C-terminal domain of the p63 gene can cause ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome, a life-threatening disorder characterized by skin fragility...

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Autores principales: Russo, Claudia, Osterburg, Christian, Sirico, Anna, Antonini, Dario, Ambrosio, Raffaele, Würz, Julia Maren, Rinnenthal, Jörg, Ferniani, Marco, Kehrloesser, Sebastian, Schäfer, Birgit, Güntert, Peter, Sinha, Satrajit, Dötsch, Volker, Missero, Caterina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: National Academy of Sciences 2018
Materias:
PNAS Plus
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5798343/
https://www.ncbi.nlm.nih.gov/pubmed/29339502
http://dx.doi.org/10.1073/pnas.1713773115
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author Russo, Claudia
Osterburg, Christian
Sirico, Anna
Antonini, Dario
Ambrosio, Raffaele
Würz, Julia Maren
Rinnenthal, Jörg
Ferniani, Marco
Kehrloesser, Sebastian
Schäfer, Birgit
Güntert, Peter
Sinha, Satrajit
Dötsch, Volker
Missero, Caterina
author_facet Russo, Claudia
Osterburg, Christian
Sirico, Anna
Antonini, Dario
Ambrosio, Raffaele
Würz, Julia Maren
Rinnenthal, Jörg
Ferniani, Marco
Kehrloesser, Sebastian
Schäfer, Birgit
Güntert, Peter
Sinha, Satrajit
Dötsch, Volker
Missero, Caterina
author_sort Russo, Claudia
collection PubMed
description The p63 gene encodes a master regulator of epidermal commitment, development, and differentiation. Heterozygous mutations in the C-terminal domain of the p63 gene can cause ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome, a life-threatening disorder characterized by skin fragility and severe, long-lasting skin erosions. Despite deep knowledge of p63 functions, little is known about mechanisms underlying disease pathology and possible treatments. Here, we show that multiple AEC-associated p63 mutations, but not those causative of other diseases, lead to thermodynamic protein destabilization, misfolding, and aggregation, similar to the known p53 gain-of-function mutants found in cancer. AEC mutant proteins exhibit impaired DNA binding and transcriptional activity, leading to dominant negative effects due to coaggregation with wild-type p63 and p73. Importantly, p63 aggregation occurs also in a conditional knock-in mouse model for the disorder, in which the misfolded p63 mutant protein leads to severe epidermal defects. Variants of p63 that abolish aggregation of the mutant proteins are able to rescue p63’s transcriptional function in reporter assays as well as in a human fibroblast-to-keratinocyte conversion assay. Our studies reveal that AEC syndrome is a protein aggregation disorder and opens avenues for therapeutic intervention.
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spelling pubmed-57983432018-02-06 Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome Russo, Claudia Osterburg, Christian Sirico, Anna Antonini, Dario Ambrosio, Raffaele Würz, Julia Maren Rinnenthal, Jörg Ferniani, Marco Kehrloesser, Sebastian Schäfer, Birgit Güntert, Peter Sinha, Satrajit Dötsch, Volker Missero, Caterina Proc Natl Acad Sci U S A PNAS Plus The p63 gene encodes a master regulator of epidermal commitment, development, and differentiation. Heterozygous mutations in the C-terminal domain of the p63 gene can cause ankyloblepharon-ectodermal defects-cleft lip/palate (AEC) syndrome, a life-threatening disorder characterized by skin fragility and severe, long-lasting skin erosions. Despite deep knowledge of p63 functions, little is known about mechanisms underlying disease pathology and possible treatments. Here, we show that multiple AEC-associated p63 mutations, but not those causative of other diseases, lead to thermodynamic protein destabilization, misfolding, and aggregation, similar to the known p53 gain-of-function mutants found in cancer. AEC mutant proteins exhibit impaired DNA binding and transcriptional activity, leading to dominant negative effects due to coaggregation with wild-type p63 and p73. Importantly, p63 aggregation occurs also in a conditional knock-in mouse model for the disorder, in which the misfolded p63 mutant protein leads to severe epidermal defects. Variants of p63 that abolish aggregation of the mutant proteins are able to rescue p63’s transcriptional function in reporter assays as well as in a human fibroblast-to-keratinocyte conversion assay. Our studies reveal that AEC syndrome is a protein aggregation disorder and opens avenues for therapeutic intervention. National Academy of Sciences 2018-01-30 2018-01-16 /pmc/articles/PMC5798343/ /pubmed/29339502 http://dx.doi.org/10.1073/pnas.1713773115 Text en Copyright © 2018 the Author(s). Published by PNAS. https://creativecommons.org/licenses/by-nc-nd/4.0/ This open access article is distributed under Creative Commons Attribution-NonCommercial-NoDerivatives License 4.0 (CC BY-NC-ND) (https://creativecommons.org/licenses/by-nc-nd/4.0/) .
spellingShingle PNAS Plus
Russo, Claudia
Osterburg, Christian
Sirico, Anna
Antonini, Dario
Ambrosio, Raffaele
Würz, Julia Maren
Rinnenthal, Jörg
Ferniani, Marco
Kehrloesser, Sebastian
Schäfer, Birgit
Güntert, Peter
Sinha, Satrajit
Dötsch, Volker
Missero, Caterina
Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome
title Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome
title_full Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome
title_fullStr Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome
title_full_unstemmed Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome
title_short Protein aggregation of the p63 transcription factor underlies severe skin fragility in AEC syndrome
title_sort protein aggregation of the p63 transcription factor underlies severe skin fragility in aec syndrome
topic PNAS Plus
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5798343/
https://www.ncbi.nlm.nih.gov/pubmed/29339502
http://dx.doi.org/10.1073/pnas.1713773115
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