Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood

Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood

Abstract Postzygotic mosaicism (PZM) in NIPBL is a strong source of causality for Cornelia de Lange syndrome (CdLS) that can have major clinical implications. Here, we further delineate the role of somatic mosaicism in CdLS by describing a series of 11 unreported patients with mosaic disease-causing...

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Main Authors: Ana Latorre-Pellicer, Marta Gil-Salvador, Ilaria Parenti, Cristina Lucia-Campos, Laura Trujillano, Iñigo Marcos-Alcalde, María Arnedo, Ángela Ascaso, Ariadna Ayerza-Casas, Rebeca Antoñanzas-Pérez, Cristina Gervasini, Maria Piccione, Milena Mariani, Axel Weber, Deniz Kanber, Alma Kuechler, Martin Munteanu, Katharina Khuller, Gloria Bueno-Lozano, Beatriz Puisac, Paulino Gómez-Puertas, Angelo Selicorni, Frank J. Kaiser, Feliciano J. Ramos, Juan Pié
Format: Article
Language:English
Published: Nature Publishing Group 2021-07-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-94958-z
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author Ana Latorre-Pellicer
Marta Gil-Salvador
Ilaria Parenti
Cristina Lucia-Campos
Laura Trujillano
Iñigo Marcos-Alcalde
María Arnedo
Ángela Ascaso
Ariadna Ayerza-Casas
Rebeca Antoñanzas-Pérez
Cristina Gervasini
Maria Piccione
Milena Mariani
Axel Weber
Deniz Kanber
Alma Kuechler
Martin Munteanu
Katharina Khuller
Gloria Bueno-Lozano
Beatriz Puisac
Paulino Gómez-Puertas
Angelo Selicorni
Frank J. Kaiser
Feliciano J. Ramos
Juan Pié
spellingShingle Ana Latorre-Pellicer
Marta Gil-Salvador
Ilaria Parenti
Cristina Lucia-Campos
Laura Trujillano
Iñigo Marcos-Alcalde
María Arnedo
Ángela Ascaso
Ariadna Ayerza-Casas
Rebeca Antoñanzas-Pérez
Cristina Gervasini
Maria Piccione
Milena Mariani
Axel Weber
Deniz Kanber
Alma Kuechler
Martin Munteanu
Katharina Khuller
Gloria Bueno-Lozano
Beatriz Puisac
Paulino Gómez-Puertas
Angelo Selicorni
Frank J. Kaiser
Feliciano J. Ramos
Juan Pié
Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood
Scientific Reports
author_facet Ana Latorre-Pellicer
Marta Gil-Salvador
Ilaria Parenti
Cristina Lucia-Campos
Laura Trujillano
Iñigo Marcos-Alcalde
María Arnedo
Ángela Ascaso
Ariadna Ayerza-Casas
Rebeca Antoñanzas-Pérez
Cristina Gervasini
Maria Piccione
Milena Mariani
Axel Weber
Deniz Kanber
Alma Kuechler
Martin Munteanu
Katharina Khuller
Gloria Bueno-Lozano
Beatriz Puisac
Paulino Gómez-Puertas
Angelo Selicorni
Frank J. Kaiser
Feliciano J. Ramos
Juan Pié
author_sort Ana Latorre-Pellicer
title Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood
title_short Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood
title_full Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood
title_fullStr Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood
title_full_unstemmed Clinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in blood
title_sort clinical relevance of postzygotic mosaicism in cornelia de lange syndrome and purifying selection of nipbl variants in blood
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-07-01
description Abstract Postzygotic mosaicism (PZM) in NIPBL is a strong source of causality for Cornelia de Lange syndrome (CdLS) that can have major clinical implications. Here, we further delineate the role of somatic mosaicism in CdLS by describing a series of 11 unreported patients with mosaic disease-causing variants in NIPBL and performing a retrospective cohort study from a Spanish CdLS diagnostic center. By reviewing the literature and combining our findings with previously published data, we demonstrate a negative selection against somatic deleterious NIPBL variants in blood. Furthermore, the analysis of all reported cases indicates an unusual high prevalence of mosaicism in CdLS, occurring in 13.1% of patients with a positive molecular diagnosis. It is worth noting that most of the affected individuals with mosaicism have a clinical phenotype at least as severe as those with constitutive pathogenic variants. However, the type of genetic change does not vary between germline and somatic events and, even in the presence of mosaicism, missense substitutions are located preferentially within the HEAT repeat domain of NIPBL. In conclusion, the high prevalence of mosaicism in CdLS as well as the disparity in tissue distribution provide a novel orientation for the clinical management and genetic counselling of families.
url https://doi.org/10.1038/s41598-021-94958-z
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spelling doaj-44bd90137bd44131872e1f1eb901a15b2021-08-01T11:25:59ZengNature Publishing GroupScientific Reports2045-23222021-07-0111111110.1038/s41598-021-94958-zClinical relevance of postzygotic mosaicism in Cornelia de Lange syndrome and purifying selection of NIPBL variants in bloodAna Latorre-Pellicer0Marta Gil-Salvador1Ilaria Parenti2Cristina Lucia-Campos3Laura Trujillano4Iñigo Marcos-Alcalde5María Arnedo6Ángela Ascaso7Ariadna Ayerza-Casas8Rebeca Antoñanzas-Pérez9Cristina Gervasini10Maria Piccione11Milena Mariani12Axel Weber13Deniz Kanber14Alma Kuechler15Martin Munteanu16Katharina Khuller17Gloria Bueno-Lozano18Beatriz Puisac19Paulino Gómez-Puertas20Angelo Selicorni21Frank J. Kaiser22Feliciano J. Ramos23Juan Pié24Unit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonUnit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonInstitut für Humangenetik, Universitätsklinikum Essen, Universität Duisburg-EssenUnit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonUnit of Clinical Genetics, Service of Paediatrics, Hospital Clínico Universitario Lozano Blesa, Department of Paediatrics, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonMolecular Modelling Group, Centro de Biología Molecular Severo Ochoa, CBMSO (CSIC-UAM)Unit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonUnit of Clinical Genetics, Service of Paediatrics, Hospital Clínico Universitario Lozano Blesa, Department of Paediatrics, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonUnit of Paediatric Cardiology, Service of Paediatrics, Hospital Universitario Miguel ServetUnit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonGenetica Medica, Dipartimento di Scienze della Salute, Università degli Studi di MilanoDepartment of Health Promotion, Mother and Child Care, Internal Medicine and Medical Specialties, University of PalermoCentro Fondazione Mariani per il Bambino Fragile, Department of Pediatrics, ASST-Lariana Sant’Anna HospitalInstitute of Human Genetics, Justus-Liebig-UniversityInstitut für Humangenetik, Universitätsklinikum Essen, Universität Duisburg-EssenInstitut für Humangenetik, Universitätsklinikum Essen, Universität Duisburg-EssenInstitut für Humangenetik, Universitätsklinikum Essen, Universität Duisburg-EssenInstitut für Humangenetik, Universitätsklinikum Essen, Universität Duisburg-EssenUnit of Clinical Genetics, Service of Paediatrics, Hospital Clínico Universitario Lozano Blesa, Department of Paediatrics, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonUnit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonMolecular Modelling Group, Centro de Biología Molecular Severo Ochoa, CBMSO (CSIC-UAM)Centro Fondazione Mariani per il Bambino Fragile, Department of Pediatrics, ASST-Lariana Sant’Anna HospitalInstitut für Humangenetik, Universitätsklinikum Essen, Universität Duisburg-EssenUnit of Clinical Genetics, Service of Paediatrics, Hospital Clínico Universitario Lozano Blesa, Department of Paediatrics, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonUnit of Clinical Genetics and Functional Genomics, Department of Pharmacology-Physiology, School of Medicine, Universidad de Zaragoza, CIBERER-GCV02 and IIS-AragonAbstract Postzygotic mosaicism (PZM) in NIPBL is a strong source of causality for Cornelia de Lange syndrome (CdLS) that can have major clinical implications. Here, we further delineate the role of somatic mosaicism in CdLS by describing a series of 11 unreported patients with mosaic disease-causing variants in NIPBL and performing a retrospective cohort study from a Spanish CdLS diagnostic center. By reviewing the literature and combining our findings with previously published data, we demonstrate a negative selection against somatic deleterious NIPBL variants in blood. Furthermore, the analysis of all reported cases indicates an unusual high prevalence of mosaicism in CdLS, occurring in 13.1% of patients with a positive molecular diagnosis. It is worth noting that most of the affected individuals with mosaicism have a clinical phenotype at least as severe as those with constitutive pathogenic variants. However, the type of genetic change does not vary between germline and somatic events and, even in the presence of mosaicism, missense substitutions are located preferentially within the HEAT repeat domain of NIPBL. In conclusion, the high prevalence of mosaicism in CdLS as well as the disparity in tissue distribution provide a novel orientation for the clinical management and genetic counselling of families.https://doi.org/10.1038/s41598-021-94958-z

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