Identification of de novo variants in nonsyndromic cleft lip with/without cleft palate patients with low polygenic risk scores

Nina Ishorst; Leonie Henschel; Frederic Thieme; Dmitriy Drichel; Sugirthan Sivalingam; Sarah L. Mehrem; Ariane C. Fechtner; Julia Fazaal; Julia Welzenbach; André Heimbach; Carlo Maj; Oleg Borisov; Jonas Hausen; Ruth Raff; Alexander Hoischen; Michael Dixon; Alvaro Rada‐Iglesias; Michaela Bartusel; Augusto Rojas‐Martinez; Khalid Aldhorae; Bert Braumann; Teresa Kruse; Christian Kirschneck; Gerrit Spanier; Heiko Reutter; Stefanie Nowak; Lina Gölz; Michael Knapp; Andreas Buness; Peter Krawitz; Markus M. Nöthen; Michael Nothnagel; Tim Becker; Kerstin U. Ludwig; Elisabeth Mangold

doi:10.1002/mgg3.2109

Molecular Genetics & Genomic Medicine (Mar 2023)

Identification of de novo variants in nonsyndromic cleft lip with/without cleft palate patients with low polygenic risk scores

Nina Ishorst,
Leonie Henschel,
Frederic Thieme,
Dmitriy Drichel,
Sugirthan Sivalingam,
Sarah L. Mehrem,
Ariane C. Fechtner,
Julia Fazaal,
Julia Welzenbach,
André Heimbach,
Carlo Maj,
Oleg Borisov,
Jonas Hausen,
Ruth Raff,
Alexander Hoischen,
Michael Dixon,
Alvaro Rada‐Iglesias,
Michaela Bartusel,
Augusto Rojas‐Martinez,
Khalid Aldhorae,
Bert Braumann,
Teresa Kruse,
Christian Kirschneck,
Gerrit Spanier,
Heiko Reutter,
Stefanie Nowak,
Lina Gölz,
Michael Knapp,
Andreas Buness,
Peter Krawitz,
Markus M. Nöthen,
Michael Nothnagel,
Tim Becker,
Kerstin U. Ludwig,
Elisabeth Mangold

Affiliations

Nina Ishorst: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Leonie Henschel: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Frederic Thieme: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Dmitriy Drichel: Cologne Center for Genomics University of Cologne Cologne Germany
Sugirthan Sivalingam: Core Unit for Bioinformatic Analysis, Medical Faculty University of Bonn Bonn Germany
Sarah L. Mehrem: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Ariane C. Fechtner: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Julia Fazaal: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Julia Welzenbach: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
André Heimbach: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Carlo Maj: Institute for Genomic Statistics and Bioinformatics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Oleg Borisov: Institute for Genomic Statistics and Bioinformatics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Jonas Hausen: Core Unit for Bioinformatic Analysis, Medical Faculty University of Bonn Bonn Germany
Ruth Raff: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Alexander Hoischen: Department of Human Genetics Radboud University Medical Center Nijmegen The Netherlands
Michael Dixon: Faculty of Biology, Medicine & Health University of Manchester Manchester UK
Alvaro Rada‐Iglesias: Institute of Biomedicine and Biotechnology of Cantabria (IBBTEC) CSIC/University of Cantabria Santander Spain
Michaela Bartusel: Center for Molecular Medicine Cologne (CMMC) University of Cologne Cologne Germany
Augusto Rojas‐Martinez: Tecnologico de Monterrey Escuela de Medicina y Ciencias de la Salud Monterrey Mexico
Khalid Aldhorae: Department of Orthodontics, College of Dentistry Thamar University Thamar Yemen
Bert Braumann: Faculty of Medicine and University Hospital Cologne, Department of Orthodontics University of Cologne Cologne Germany
Teresa Kruse: Faculty of Medicine and University Hospital Cologne, Department of Orthodontics University of Cologne Cologne Germany
Christian Kirschneck: Department of Orthodontics University of Regensburg Regensburg Germany
Gerrit Spanier: Department of Cranio‐Maxillofacial Surgery University Hospital Regensburg Regensburg Germany
Heiko Reutter: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Stefanie Nowak: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Lina Gölz: Department of Orthodontics University of Erlangen‐Nürnberg Erlangen Germany
Michael Knapp: Institute of Medical Biometry, Informatics and Epidemiology University Hospital Bonn Bonn Germany
Andreas Buness: Core Unit for Bioinformatic Analysis, Medical Faculty University of Bonn Bonn Germany
Peter Krawitz: Institute for Genomic Statistics and Bioinformatics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Markus M. Nöthen: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Michael Nothnagel: Cologne Center for Genomics University of Cologne Cologne Germany
Tim Becker: Institute of Community Medicine University of Greifswald Greifswald Germany
Kerstin U. Ludwig: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany
Elisabeth Mangold: Institute of Human Genetics, University of Bonn School of Medicine & University Hospital Bonn Bonn Germany

DOI: https://doi.org/10.1002/mgg3.2109
Journal volume & issue: Vol. 11, no. 3
pp. n/a – n/a

Abstract

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Abstract Background Nonsyndromic cleft lip with/without cleft palate (nsCL/P) is a congenital malformation of multifactorial etiology. Research has identified >40 genome‐wide significant risk loci, which explain less than 40% of nsCL/P heritability. Studies show that some of the hidden heritability is explained by rare penetrant variants. Methods To identify new candidate genes, we searched for highly penetrant de novo variants (DNVs) in 50 nsCL/P patient/parent‐trios with a low polygenic risk for the phenotype (discovery). We prioritized DNV‐carrying candidate genes from the discovery for resequencing in independent cohorts of 1010 nsCL/P patients of diverse ethnicities and 1574 population‐matched controls (replication). Segregation analyses and rare variant association in the replication cohort, in combination with additional data (genome‐wide association data, expression, protein–protein‐interactions), were used for final prioritization. Conclusion In the discovery step, 60 DNVs were identified in 60 genes, including a variant in the established nsCL/P risk gene CDH1. Re‐sequencing of 32 prioritized genes led to the identification of 373 rare, likely pathogenic variants. Finally, MDN1 and PAXIP1 were prioritized as top candidates. Our findings demonstrate that DNV detection, including polygenic risk score analysis, is a powerful tool for identifying nsCL/P candidate genes, which can also be applied to other multifactorial congenital malformations.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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