Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype

Craniosynostosis are a heterogeneous group of genetic conditions characterized by the premature fusion of the skull bones. The most common forms of craniosynostosis are Crouzon, Apert and Pfeiffer syndromes. They differ from each other in various additional clinical manifestations, e.g., syndactyly...

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Autores principales: Lo Vecchio, Filomena, Tabolacci, Elisabetta, Nobile, Veronica, Pomponi, Maria Grazia, Pietrobono, Roberta, Neri, Giovanni, Amenta, Simona, Candida, Ettore, Grippaudo, Cristina, Lo Cascio, Ettore, Vita, Alessia, Tiberio, Federica, Arcovito, Alessandro, Lattanzi, Wanda, Genuardi, Maurizio, Chiurazzi, Pietro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9319849/
https://www.ncbi.nlm.nih.gov/pubmed/35885943
http://dx.doi.org/10.3390/genes13071161
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author Lo Vecchio, Filomena
Tabolacci, Elisabetta
Nobile, Veronica
Pomponi, Maria Grazia
Pietrobono, Roberta
Neri, Giovanni
Amenta, Simona
Candida, Ettore
Grippaudo, Cristina
Lo Cascio, Ettore
Vita, Alessia
Tiberio, Federica
Arcovito, Alessandro
Lattanzi, Wanda
Genuardi, Maurizio
Chiurazzi, Pietro
author_facet Lo Vecchio, Filomena
Tabolacci, Elisabetta
Nobile, Veronica
Pomponi, Maria Grazia
Pietrobono, Roberta
Neri, Giovanni
Amenta, Simona
Candida, Ettore
Grippaudo, Cristina
Lo Cascio, Ettore
Vita, Alessia
Tiberio, Federica
Arcovito, Alessandro
Lattanzi, Wanda
Genuardi, Maurizio
Chiurazzi, Pietro
author_sort Lo Vecchio, Filomena
collection PubMed
description Craniosynostosis are a heterogeneous group of genetic conditions characterized by the premature fusion of the skull bones. The most common forms of craniosynostosis are Crouzon, Apert and Pfeiffer syndromes. They differ from each other in various additional clinical manifestations, e.g., syndactyly is typical of Apert and rare in Pfeiffer syndrome. Their inheritance is autosomal dominant with incomplete penetrance and one of the main genes responsible for these syndromes is FGFR2, mapped on chromosome 10, encoding fibroblast growth factor receptor 2. We report an FGFR2 gene variant in a mother and daughter who present with different clinical features of Crouzon syndrome. The daughter is more severely affected than her mother, as also verified by a careful study of the face and oral cavity. The c.1032G>A transition in exon 8, already reported as a synonymous p.Ala344 = variant in Crouzon patients, also activates a new donor splice site leading to the loss of 51 nucleotides and the in-frame removal of 17 amino acids. We observed lower FGFR2 transcriptional and translational levels in the daughter compared to the mother and healthy controls. A preliminary functional assay and a molecular modeling added further details to explain the discordant phenotype of the two patients.
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spelling pubmed-93198492022-07-27 Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype Lo Vecchio, Filomena Tabolacci, Elisabetta Nobile, Veronica Pomponi, Maria Grazia Pietrobono, Roberta Neri, Giovanni Amenta, Simona Candida, Ettore Grippaudo, Cristina Lo Cascio, Ettore Vita, Alessia Tiberio, Federica Arcovito, Alessandro Lattanzi, Wanda Genuardi, Maurizio Chiurazzi, Pietro Genes (Basel) Article Craniosynostosis are a heterogeneous group of genetic conditions characterized by the premature fusion of the skull bones. The most common forms of craniosynostosis are Crouzon, Apert and Pfeiffer syndromes. They differ from each other in various additional clinical manifestations, e.g., syndactyly is typical of Apert and rare in Pfeiffer syndrome. Their inheritance is autosomal dominant with incomplete penetrance and one of the main genes responsible for these syndromes is FGFR2, mapped on chromosome 10, encoding fibroblast growth factor receptor 2. We report an FGFR2 gene variant in a mother and daughter who present with different clinical features of Crouzon syndrome. The daughter is more severely affected than her mother, as also verified by a careful study of the face and oral cavity. The c.1032G>A transition in exon 8, already reported as a synonymous p.Ala344 = variant in Crouzon patients, also activates a new donor splice site leading to the loss of 51 nucleotides and the in-frame removal of 17 amino acids. We observed lower FGFR2 transcriptional and translational levels in the daughter compared to the mother and healthy controls. A preliminary functional assay and a molecular modeling added further details to explain the discordant phenotype of the two patients. MDPI 2022-06-27 /pmc/articles/PMC9319849/ /pubmed/35885943 http://dx.doi.org/10.3390/genes13071161 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lo Vecchio, Filomena
Tabolacci, Elisabetta
Nobile, Veronica
Pomponi, Maria Grazia
Pietrobono, Roberta
Neri, Giovanni
Amenta, Simona
Candida, Ettore
Grippaudo, Cristina
Lo Cascio, Ettore
Vita, Alessia
Tiberio, Federica
Arcovito, Alessandro
Lattanzi, Wanda
Genuardi, Maurizio
Chiurazzi, Pietro
Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype
title Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype
title_full Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype
title_fullStr Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype
title_full_unstemmed Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype
title_short Mother and Daughter Carrying of the Same Pathogenic Variant in FGFR2 with Discordant Phenotype
title_sort mother and daughter carrying of the same pathogenic variant in fgfr2 with discordant phenotype
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9319849/
https://www.ncbi.nlm.nih.gov/pubmed/35885943
http://dx.doi.org/10.3390/genes13071161
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