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

APA

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 (2018-10 ) .Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia.

ISO 690

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. 2018-10 .Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia.

https://hdl.handle.net/20.500.12080/39723

EndNote

Mendeley

dc.contributor.author	Tarilonte, María
dc.contributor.author	Morín, Matías
dc.contributor.author	Ramos, Patricia
dc.contributor.author	Galdós, Marta
dc.contributor.author	Blanco Kelly, Fiona
dc.contributor.author	Villaverde, Cristina
dc.contributor.author	Rey Zamora, Dolores
dc.contributor.author	Rebolleda, Gema
dc.contributor.author	Muñoz Negrete, Francisco J.
dc.contributor.author	Tahsin Swafiri, Saoud
dc.contributor.author	Gener, Blanca
dc.contributor.author	Moreno Pelayo, Miguel Angel
dc.contributor.author	Ayuso, Carmen
dc.contributor.author	Villamar, Manuela
dc.contributor.author	Corton, Marta
dc.date.accessioned	2024-02-12T14:38:34Z
dc.date.available	2024-02-12T14:38:34Z
dc.date.created	2018-10
dc.date.issued	2018-10
dc.identifier.uri	https://hdl.handle.net/20.500.12080/39723
dc.description.abstract	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.	es_ES
dc.format	application/pdf	es_ES
dc.language	eng	es_ES
dc.rights	CC-BY	es_ES
dc.rights.uri	http://creativecommons.org/licenses/by/4.0/deed.es	es_ES
dc.title	Parental Mosaicism in PAX6 Causes Intra-Familial Variability: Implications for Genetic Counseling of Congenital Aniridia and Microphthalmia	es_ES
dc.type	info:eu-repo/semantics/article	es_ES
dc.rights.accessrights	info:eu-repo/semantics/openAccess	es_ES
dc.identifier.location	N/A	es_ES