| Literature DB >> 34176129 |
Jonathan Lévy1, Bérénice Schell1, Hala Nasser1, Myriam Rachid1, Lyse Ruaud1,2,3, Nathalie Couque1, Patrick Callier4,5,6, Laurence Faivre4,6, Nathalie Marle5,6, Aafke Engwerda7, Conny M A van Ravenswaaij-Arts7, Morgane Plutino8, Houda Karmous-Benailly8, Caroline Benech9, Sylvia Redon10, Odile Boute11, Elise Boudry Labis12, Mélanie Rama12, Paul Kuentz6,13, Jessica Assoumani14, Lionel Van Maldergem14,15, Céline Dupont1, Alain Verloes1,2,3, Anne-Claude Tabet1,16.
Abstract
Ephrin receptor and their ligands, the ephrins, are widely expressed in the developing brain. They are implicated in several developmental processes that are crucial for brain development. Deletions in genes encoding for members of the Eph/ephrin receptor family were reported in several neurodevelopmental disorders. The ephrin receptor A7 gene (EPHA7) encodes a member of ephrin receptor subfamily of the protein-tyrosine kinase family. EPHA7 plays a role in corticogenesis processes, determines brain size and shape, and is involved in development of the central nervous system. One patient only was reported so far with a de novo deletion encompassing EPHA7 in 6q16.1. We report 12 additional patients from nine unrelated pedigrees with similar deletions. The deletions were inherited in nine out of 12 patients, suggesting variable expressivity and incomplete penetrance. Four patients had tiny deletions involving only EPHA7, suggesting a critical role of EPHA7 in a neurodevelopmental disability phenotype. We provide further evidence for EPHA7 deletion as a risk factor for neurodevelopmental disorder and delineate its clinical phenotype.Entities:
Keywords: 6q16.1 microdeletion; EPHA7; intellectual disability; microcephaly; neurodevelopmental disorder; speech and language development
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Year: 2021 PMID: 34176129 DOI: 10.1111/cge.14017
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438