| Literature DB >> 31585109 |
Andrea Accogli1, Sara Calabretta2, Judith St-Onge3, Nassima Boudrahem-Addour3, Alexandre Dionne-Laporte4, Pascal Joset5, Silvia Azzarello-Burri5, Anita Rauch5, Joel Krier6, Elizabeth Fieg6, Juan C Pallais6, Allyn McConkie-Rosell7, Marie McDonald7, Sharon F Freedman8, Jean-Baptiste Rivière3, Joël Lafond-Lapalme3, Brittany N Simpson9, Robert J Hopkin9, Aurélien Trimouille10, Julien Van-Gils10, Amber Begtrup11, Kirsty McWalter11, Heron Delphine12, Boris Keren12, David Genevieve13, Emanuela Argilli14, Elliott H Sherr14, Mariasavina Severino15, Guy A Rouleau16, Patricia T Yam2, Frédéric Charron17, Myriam Srour18.
Abstract
Cadherins constitute a family of transmembrane proteins that mediate calcium-dependent cell-cell adhesion. The extracellular domain of cadherins consists of extracellular cadherin (EC) domains, separated by calcium binding sites. The EC interacts with other cadherin molecules in cis and in trans to mechanically hold apposing cell surfaces together. CDH2 encodes N-cadherin, whose essential roles in neural development include neuronal migration and axon pathfinding. However, CDH2 has not yet been linked to a Mendelian neurodevelopmental disorder. Here, we report de novo heterozygous pathogenic variants (seven missense, two frameshift) in CDH2 in nine individuals with a syndromic neurodevelopmental disorder characterized by global developmental delay and/or intellectual disability, variable axon pathfinding defects (corpus callosum agenesis or hypoplasia, mirror movements, Duane anomaly), and ocular, cardiac, and genital anomalies. All seven missense variants (c.1057G>A [p.Asp353Asn]; c.1789G>A [p.Asp597Asn]; c.1789G>T [p.Asp597Tyr]; c.1802A>C [p.Asn601Thr]; c.1839C>G [p.Cys613Trp]; c.1880A>G [p.Asp627Gly]; c.2027A>G [p.Tyr676Cys]) result in substitution of highly conserved residues, and six of seven cluster within EC domains 4 and 5. Four of the substitutions affect the calcium-binding site in the EC4-EC5 interdomain. We show that cells expressing these variants in the EC4-EC5 domains have a defect in cell-cell adhesion; this defect includes impaired binding in trans with N-cadherin-WT expressed on apposing cells. The two frameshift variants (c.2563_2564delCT [p.Leu855Valfs∗4]; c.2564_2567dupTGTT [p.Leu856Phefs∗5]) are predicted to lead to a truncated cytoplasmic domain. Our study demonstrates that de novo heterozygous variants in CDH2 impair the adhesive activity of N-cadherin, resulting in a multisystemic developmental disorder, that could be named ACOG syndrome (agenesis of corpus callosum, axon pathfinding, cardiac, ocular, and genital defects).Entities:
Keywords: ACOG; CDH2; N-cadherin; cardiac defects; cell-cell adhesion; corpus callosum; eye defects; genital defects; intellectual disability
Mesh:
Substances:
Year: 2019 PMID: 31585109 PMCID: PMC6817525 DOI: 10.1016/j.ajhg.2019.09.005
Source DB: PubMed Journal: Am J Hum Genet ISSN: 0002-9297 Impact factor: 11.043