Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia

Mutations in PAX6 are involved in several developmental eye disorders. These disorders have considerable phenotypic variability, ranging from panocular forms of congenital aniridia and microphthalmia to isolated anomalies of the anterior or posterior segment. Here, we describe 3 families with variab...

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Autores principales: Tarilonte, María, Morín, Matías, Ramos, Patricia, Galdós, Marta, Blanco-Kelly, Fiona, Villaverde, Cristina, Rey-Zamora, Dolores, Rebolleda, Gema, Muñoz-Negrete, Francisco J., Tahsin-Swafiri, Saoud, Gener, Blanca, Moreno-Pelayo, Miguel-Angel, Ayuso, Carmen, Villamar, Manuela, Corton, Marta
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Genetics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6199369/
https://www.ncbi.nlm.nih.gov/pubmed/30386378
http://dx.doi.org/10.3389/fgene.2018.00479
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author Tarilonte, María
Morín, Matías
Ramos, Patricia
Galdós, Marta
Blanco-Kelly, Fiona
Villaverde, Cristina
Rey-Zamora, Dolores
Rebolleda, Gema
Muñoz-Negrete, Francisco J.
Tahsin-Swafiri, Saoud
Gener, Blanca
Moreno-Pelayo, Miguel-Angel
Ayuso, Carmen
Villamar, Manuela
Corton, Marta
author_facet Tarilonte, María
Morín, Matías
Ramos, Patricia
Galdós, Marta
Blanco-Kelly, Fiona
Villaverde, Cristina
Rey-Zamora, Dolores
Rebolleda, Gema
Muñoz-Negrete, Francisco J.
Tahsin-Swafiri, Saoud
Gener, Blanca
Moreno-Pelayo, Miguel-Angel
Ayuso, Carmen
Villamar, Manuela
Corton, Marta
author_sort Tarilonte, María
collection PubMed
description Mutations in PAX6 are involved in several developmental eye disorders. These disorders have considerable phenotypic variability, ranging from panocular forms of congenital aniridia and microphthalmia to isolated anomalies of the anterior or posterior segment. Here, we describe 3 families with variable inter-generational ocular expression of aniridia, iris coloboma, or microphthalmia, and an unusual transmission of PAX6 mutations from an unaffected or mildly affected parent; all of which raised suspicion of gonosomal mosaicism. We first identified two previously known nonsense mutations and one novel likely pathogenic missense variant in PAX6 in probands by means of targeted NGS. The subsequent segregation analysis by Sanger sequencing evidenced the presence of highly probable mosaic events in paternal blood samples. Mosaicism was further confirmed by droplet digital PCR analysis in several somatic tissues of mosaic fathers. Quantification of the mutant allele fraction in parental samples showed a marked deviation from 50%, with a range between 12 and 29% depending on cell type. Gonosomal mosaicsm was definitively confirmed in one of the families thanks to the availability of a sperm sample from the mosaic father. Thus, the recurrence risk in this family was estimated to be about one-third. This is the first report confirming parental PAX6 mosaicism as a cause of disease recurrence in aniridia and other related phenotypes. In addition, we demonstrated that post-zygotic mosaicism is a frequent and underestimated pathogenic mechanism in aniridia, explaining intra-familial phenotypic variability in many cases. Our findings may have substantial implications for genetic counseling in congenital aniridia. Thus, we also highlight the importance of comprehensive genetic screening of parents for new sporadic cases with aniridia or related developmental eye disease to more accurately assess recurrence risk. In conclusion, somatic and/or gonosomal mosaicism should be taken into consideration as a genetic factor to explain not only families with unaffected parents despite multiple affected children but also variable expressivity, apparent de novo cases, and even uncharacterized cases of aniridia and related developmental eye disorders, apparently lacking PAX6 mutations.
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spelling pubmed-61993692018-11-01 Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia Tarilonte, María Morín, Matías Ramos, Patricia Galdós, Marta Blanco-Kelly, Fiona Villaverde, Cristina Rey-Zamora, Dolores Rebolleda, Gema Muñoz-Negrete, Francisco J. Tahsin-Swafiri, Saoud Gener, Blanca Moreno-Pelayo, Miguel-Angel Ayuso, Carmen Villamar, Manuela Corton, Marta Front Genet Genetics Mutations in PAX6 are involved in several developmental eye disorders. These disorders have considerable phenotypic variability, ranging from panocular forms of congenital aniridia and microphthalmia to isolated anomalies of the anterior or posterior segment. Here, we describe 3 families with variable inter-generational ocular expression of aniridia, iris coloboma, or microphthalmia, and an unusual transmission of PAX6 mutations from an unaffected or mildly affected parent; all of which raised suspicion of gonosomal mosaicism. We first identified two previously known nonsense mutations and one novel likely pathogenic missense variant in PAX6 in probands by means of targeted NGS. The subsequent segregation analysis by Sanger sequencing evidenced the presence of highly probable mosaic events in paternal blood samples. Mosaicism was further confirmed by droplet digital PCR analysis in several somatic tissues of mosaic fathers. Quantification of the mutant allele fraction in parental samples showed a marked deviation from 50%, with a range between 12 and 29% depending on cell type. Gonosomal mosaicsm was definitively confirmed in one of the families thanks to the availability of a sperm sample from the mosaic father. Thus, the recurrence risk in this family was estimated to be about one-third. This is the first report confirming parental PAX6 mosaicism as a cause of disease recurrence in aniridia and other related phenotypes. In addition, we demonstrated that post-zygotic mosaicism is a frequent and underestimated pathogenic mechanism in aniridia, explaining intra-familial phenotypic variability in many cases. Our findings may have substantial implications for genetic counseling in congenital aniridia. Thus, we also highlight the importance of comprehensive genetic screening of parents for new sporadic cases with aniridia or related developmental eye disease to more accurately assess recurrence risk. In conclusion, somatic and/or gonosomal mosaicism should be taken into consideration as a genetic factor to explain not only families with unaffected parents despite multiple affected children but also variable expressivity, apparent de novo cases, and even uncharacterized cases of aniridia and related developmental eye disorders, apparently lacking PAX6 mutations. Frontiers Media S.A. 2018-10-17 /pmc/articles/PMC6199369/ /pubmed/30386378 http://dx.doi.org/10.3389/fgene.2018.00479 Text en Copyright © 2018 Tarilonte, Morín, Ramos, Galdós, Blanco-Kelly, Villaverde, Rey-Zamora, Rebolleda, Muñoz-Negrete, Tahsin-Swafiri, Gener, Moreno-Pelayo, Ayuso, Villamar and Corton. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Genetics
Tarilonte, María
Morín, Matías
Ramos, Patricia
Galdós, Marta
Blanco-Kelly, Fiona
Villaverde, Cristina
Rey-Zamora, Dolores
Rebolleda, Gema
Muñoz-Negrete, Francisco J.
Tahsin-Swafiri, Saoud
Gener, Blanca
Moreno-Pelayo, Miguel-Angel
Ayuso, Carmen
Villamar, Manuela
Corton, Marta
Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia
title Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia
title_full Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia
title_fullStr Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia
title_full_unstemmed Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia
title_short Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia
title_sort parental mosaicism in pax6 causes intra-familial variability: implications for genetic counseling of congenital aniridia and microphthalmia
topic Genetics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6199369/
https://www.ncbi.nlm.nih.gov/pubmed/30386378
http://dx.doi.org/10.3389/fgene.2018.00479
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