Next‐generation phenotyping in Nigerian children with Cornelia de Lange syndrome

Author:

Arlt Annabelle1ORCID,Knaus Alexej1ORCID,Hsieh Tzung‐Chien1ORCID,Klinkhammer Hannah12ORCID,Bhasin Meghna Ahuja1ORCID,Hustinx Alexander1ORCID,Moosa Shahida3ORCID,Krawitz Peter1ORCID,Ekure Ekanem4ORCID

Affiliation:

1. Institute for Genomic Statistics and Bioinformatics, University Hospital Bonn Bonn Germany

2. Institute for Medical Biometry, Informatics and Epidemiology, University Hospital Bonn Bonn Germany

3. Division of Molecular Biology and Human Genetics Stellenbosch University and Medical Genetics, Tygerberg Hospital Cape Town South Africa

4. Faculty of Clinical Sciences, Department of Pediatrics College of Medicine, University of Lagos Lagos Nigeria

Abstract

AbstractNext‐generation phenotyping (NGP) can be used to compute the similarity of dysmorphic patients to known syndromic diseases. So far, the technology has been evaluated in variant prioritization and classification, providing evidence for pathogenicity if the phenotype matched with other patients with a confirmed molecular diagnosis. In a Nigerian cohort of individuals with facial dysmorphism, we used the NGP tool GestaltMatcher to screen portraits prior to genetic testing and subjected individuals with high similarity scores to exome sequencing (ES). Here, we report on two individuals with global developmental delay, pulmonary artery stenosis, and genital and limb malformations for whom GestaltMatcher yielded Cornelia de Lange syndrome (CdLS) as the top hit. ES revealed a known pathogenic nonsense variant, NM_133433.4: c.598C>T; p.(Gln200*), as well as a novel frameshift variant c.7948dup; p.(Ile2650Asnfs*11) in NIPBL. Our results suggest that NGP can be used as a screening tool and thresholds could be defined for achieving high diagnostic yields in ES. Training the artificial intelligence (AI) with additional cases of the same ethnicity might further increase the positive predictive value of GestaltMatcher.

Publisher

Wiley

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