Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome

Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome

The 22q11.2 deletion syndrome (22q11.2DS) is the most common genomic disorder in humans and is the result of a recurrent 1.5 to 2.5 Mb deletion, encompassing approximately 20–40 genes, respectively. The clinical presentation of the typical deletion includes: Velocardiofacial, Di George, Opitz G/BBB...

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Main Authors: Kathleen Rooney, Michael A. Levy, Sadegheh Haghshenas, Jennifer Kerkhof, Daniela Rogaia, Maria Giovanna Tedesco, Valentina Imperatore, Amedea Mencarelli, Gabriella Maria Squeo, Eleonora Di Venere, Giuseppe Di Cara, Alberto Verrotti, Giuseppe Merla, Matthew L. Tedder, Barbara R. DuPont, Bekim Sadikovic, Paolo Prontera
Format: Article
Language:English
Published: MDPI AG 2021-08-01
Series:International Journal of Molecular Sciences
Subjects:
22q11.2 deletion
DNA methylation
episignature
diagnostic method
DiGeorge syndrome
Velocardiofacial syndrome
Online Access:https://www.mdpi.com/1422-0067/22/16/8611
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spelling doaj-8d2822585e6d4742b51decc5c323428d2021-08-26T13:52:03ZengMDPI AGInternational Journal of Molecular Sciences1661-65961422-00672021-08-01228611861110.3390/ijms22168611Identification of a DNA Methylation Episignature in the 22q11.2 Deletion SyndromeKathleen Rooney0Michael A. Levy1Sadegheh Haghshenas2Jennifer Kerkhof3Daniela Rogaia4Maria Giovanna Tedesco5Valentina Imperatore6Amedea Mencarelli7Gabriella Maria Squeo8Eleonora Di Venere9Giuseppe Di Cara10Alberto Verrotti11Giuseppe Merla12Matthew L. Tedder13Barbara R. DuPont14Bekim Sadikovic15Paolo Prontera16Department of Pathology and Laboratory Medicine, Western University, London, ON N6A 3K7, CanadaVerspeeten Clinical Genome Centre, London Health Sciences Centre, London, ON N6A 5W9, CanadaDepartment of Pathology and Laboratory Medicine, Western University, London, ON N6A 3K7, CanadaVerspeeten Clinical Genome Centre, London Health Sciences Centre, London, ON N6A 5W9, CanadaMedical Genetics Unit, Maternal-Infantile Department, University and Hospital of Perugia, 06129 Perugia, ItalyMedical Genetics Unit, Maternal-Infantile Department, University and Hospital of Perugia, 06129 Perugia, ItalyMedical Genetics Unit, Maternal-Infantile Department, University and Hospital of Perugia, 06129 Perugia, ItalyMedical Genetics Unit, Maternal-Infantile Department, University and Hospital of Perugia, 06129 Perugia, ItalyLaboratory of Regulatory and Functional Genomics, Fondazione IRCCS Casa Sollievo della Sofferenza, 71013 San Giovanni Rotondo, ItalyLaboratory of Regulatory and Functional Genomics, Fondazione IRCCS Casa Sollievo della Sofferenza, 71013 San Giovanni Rotondo, ItalyPediatric Clinic, Department of Medicine, University of Perugia, 06129 Perugia, ItalyPediatric Clinic, Department of Medicine, University of Perugia, 06129 Perugia, ItalyLaboratory of Regulatory and Functional Genomics, Fondazione IRCCS Casa Sollievo della Sofferenza, 71013 San Giovanni Rotondo, ItalyGreenwood Genetic Center, Greenwood, SC 29646, USAGreenwood Genetic Center, Greenwood, SC 29646, USADepartment of Pathology and Laboratory Medicine, Western University, London, ON N6A 3K7, CanadaMedical Genetics Unit, Maternal-Infantile Department, University and Hospital of Perugia, 06129 Perugia, ItalyThe 22q11.2 deletion syndrome (22q11.2DS) is the most common genomic disorder in humans and is the result of a recurrent 1.5 to 2.5 Mb deletion, encompassing approximately 20–40 genes, respectively. The clinical presentation of the typical deletion includes: Velocardiofacial, Di George, Opitz G/BBB and Conotruncalanomaly face syndromes. Atypical deletions (proximal, distal or nested) are rare and characterized mainly by normal phenotype or mild intellectual disability and variable clinical features. The pathogenetic mechanisms underlying this disorder are not completely understood. Because the 22q11.2 region harbours genes coding for transcriptional factors and chromatin remodelers, in this study, we performed analysis of genome-wide DNA methylation of peripheral blood from 49 patients with 22q11.2DS using the Illumina Infinium Methylation EPIC bead chip arrays. This cohort comprises 43 typical, 2 proximal and 4 distal deletions. We demonstrated the evidence of a unique and highly specific episignature in all typical and proximal 22q11.2DS. The sensitivity and specificity of this signature was further confirmed by comparing it to over 1500 patients with other neurodevelopmental disorders with known episignatures. Mapping the 22q11.2DS DNA methylation episignature provides both novel insights into the molecular pathogenesis of this disorder and an effective tool in the molecular diagnosis of 22q11.2DS.https://www.mdpi.com/1422-0067/22/16/861122q11.2 deletionDNA methylationepisignaturediagnostic methodDiGeorge syndromeVelocardiofacial syndrome
collection DOAJ
language English
format Article
sources DOAJ
author Kathleen Rooney
Michael A. Levy
Sadegheh Haghshenas
Jennifer Kerkhof
Daniela Rogaia
Maria Giovanna Tedesco
Valentina Imperatore
Amedea Mencarelli
Gabriella Maria Squeo
Eleonora Di Venere
Giuseppe Di Cara
Alberto Verrotti
Giuseppe Merla
Matthew L. Tedder
Barbara R. DuPont
Bekim Sadikovic
Paolo Prontera
spellingShingle Kathleen Rooney
Michael A. Levy
Sadegheh Haghshenas
Jennifer Kerkhof
Daniela Rogaia
Maria Giovanna Tedesco
Valentina Imperatore
Amedea Mencarelli
Gabriella Maria Squeo
Eleonora Di Venere
Giuseppe Di Cara
Alberto Verrotti
Giuseppe Merla
Matthew L. Tedder
Barbara R. DuPont
Bekim Sadikovic
Paolo Prontera
Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome
International Journal of Molecular Sciences
22q11.2 deletion
DNA methylation
episignature
diagnostic method
DiGeorge syndrome
Velocardiofacial syndrome
author_facet Kathleen Rooney
Michael A. Levy
Sadegheh Haghshenas
Jennifer Kerkhof
Daniela Rogaia
Maria Giovanna Tedesco
Valentina Imperatore
Amedea Mencarelli
Gabriella Maria Squeo
Eleonora Di Venere
Giuseppe Di Cara
Alberto Verrotti
Giuseppe Merla
Matthew L. Tedder
Barbara R. DuPont
Bekim Sadikovic
Paolo Prontera
author_sort Kathleen Rooney
title Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome
title_short Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome
title_full Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome
title_fullStr Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome
title_full_unstemmed Identification of a DNA Methylation Episignature in the 22q11.2 Deletion Syndrome
title_sort identification of a dna methylation episignature in the 22q11.2 deletion syndrome
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1661-6596
1422-0067
publishDate 2021-08-01
description The 22q11.2 deletion syndrome (22q11.2DS) is the most common genomic disorder in humans and is the result of a recurrent 1.5 to 2.5 Mb deletion, encompassing approximately 20–40 genes, respectively. The clinical presentation of the typical deletion includes: Velocardiofacial, Di George, Opitz G/BBB and Conotruncalanomaly face syndromes. Atypical deletions (proximal, distal or nested) are rare and characterized mainly by normal phenotype or mild intellectual disability and variable clinical features. The pathogenetic mechanisms underlying this disorder are not completely understood. Because the 22q11.2 region harbours genes coding for transcriptional factors and chromatin remodelers, in this study, we performed analysis of genome-wide DNA methylation of peripheral blood from 49 patients with 22q11.2DS using the Illumina Infinium Methylation EPIC bead chip arrays. This cohort comprises 43 typical, 2 proximal and 4 distal deletions. We demonstrated the evidence of a unique and highly specific episignature in all typical and proximal 22q11.2DS. The sensitivity and specificity of this signature was further confirmed by comparing it to over 1500 patients with other neurodevelopmental disorders with known episignatures. Mapping the 22q11.2DS DNA methylation episignature provides both novel insights into the molecular pathogenesis of this disorder and an effective tool in the molecular diagnosis of 22q11.2DS.
topic 22q11.2 deletion
DNA methylation
episignature
diagnostic method
DiGeorge syndrome
Velocardiofacial syndrome
url https://www.mdpi.com/1422-0067/22/16/8611
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