Whole Exome Sequencing Is the Minimal Technological Approach in Probands Born to Consanguineous Couples

Author:

Peluso Francesca,Caraffi Stefano GiuseppeORCID,Zuntini Roberta,Trimarchi Gabriele,Ivanovski IvanORCID,Valeri Lara,Barbieri Veronica,Marinelli Maria,Pancaldi Alessia,Melli Nives,Cesario Claudia,Agolini EmanueleORCID,Cellini ElenaORCID,Radio Francesca ClementinaORCID,Crisafi Antonella,Napoli Manuela,Guerrini Renzo,Tartaglia Marco,Novelli AntonioORCID,Gargano Giancarlo,Zuffardi OrsettaORCID,Garavelli Livia

Abstract

We report on two siblings suffering from different pathogenic conditions, born to consanguineous parents. A multigene panel for brain malformations and microcephaly identified the homozygous splicing variant NM_005886.3:c.1416+1del in the KATNB1 gene in the older sister. On the other hand, exome sequencing revealed the homozygous frameshift variant NM_005245.4:c.9729del in the FAT1 gene in the younger sister, who had a more complex phenotype: in addition to bilateral anophthalmia and heart defects, she showed a right split foot with 4 toes, 5 metacarpals, second toe duplication and preaxial polydactyly on the right hand. These features have been never reported before in patients with pathogenic FAT1 variants and support the role of this gene in the development of limb buds. Notably, each parent was heterozygous for both of these variants, which were ultra-rare and rare, respectively. This study raises awareness about the value of using whole exome/genome sequencing rather than targeted gene panels when testing affected offspring born to consanguineous couples. In this way, exomic data from the parents are also made available for carrier screening, to identify heterozygous pathogenetic and likely pathogenetic variants in genes responsible for other recessive conditions, which may pose a risk for subsequent pregnancies.

Publisher

MDPI AG

Subject

Genetics (clinical),Genetics

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