DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity

Slavica Trajkova; Jennifer Kerkhof; Matteo Rossi Sebastiano; Lisa Pavinato; Enza Ferrero; Chiara Giovenino; Diana Carli; Eleonora Di Gregorio; Roberta Marinoni; Giorgia Mandrile; Flavia Palermo; Silvia Carestiato; Simona Cardaropoli; Verdiana Pullano; Antonina Rinninella; Elisa Giorgio; Tommaso Pippucci; Paola Dimartino; Jessica Rzasa; Kathleen Rooney; Haley McConkey; Aleksandar Petlichkovski; Barbara Pasini; Elena Sukarova-Angelovska; Christopher M Campbell; Kay Metcalfe; Sarah Jenkinson; Siddharth Banka; Alessandro Mussa; Giovanni Battista Ferrero; Bekim Sadikovic; Alfredo Brusco

doi:10.1016/j.xhgg.2024.100309

DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity

Slavica Trajkova, Jennifer Kerkhof, Matteo Rossi Sebastiano, Lisa Pavinato, Enza Ferrero, Chiara Giovenino, Diana Carli, Eleonora Di Gregorio, Roberta Marinoni, Giorgia Mandrile, Flavia Palermo, Silvia Carestiato, Simona Cardaropoli, Verdiana Pullano, Antonina Rinninella, Elisa Giorgio, Tommaso Pippucci, Paola Dimartino, Jessica Rzasa, Kathleen RooneyHaley McConkey, Aleksandar Petlichkovski, Barbara Pasini, Elena Sukarova-Angelovska, Christopher M Campbell, Kay Metcalfe, Sarah Jenkinson, Siddharth Banka, Alessandro Mussa, Giovanni Battista Ferrero, Bekim Sadikovic, Alfredo Brusco

Division of Evolution, Infection and Genomics

Research output: Contribution to journal › Article › peer-review

Abstract

Analysis of genomic DNA methylation by generating epigenetic signature profiles (episignatures) is increasingly being implemented in genetic diagnosis. Here we report our experience using episignature analysis to resolve both uncomplicated and complex cases of neurodevelopmental disorders (NDDs). We analyzed 97 NDDs divided into (1) a validation cohort of 59 patients with likely pathogenic/pathogenic variants characterized by a known episignature and (2) a test cohort of 38 patients harboring variants of unknown significance or unidentified variants. The expected episignature was obtained in most cases with likely pathogenic/pathogenic variants (53/59 [90%]), a revealing exception being the overlapping profile of two SMARCB1 pathogenic variants with ARID1A/B:c.6200, confirmed by the overlapping clinical features. In the test cohort, five cases showed the expected episignature, including (1) novel pathogenic variants in ARID1B and BRWD3; (2) a deletion in ATRX causing MRXFH1 X-linked mental retardation; and (3) confirmed the clinical diagnosis of Cornelia de Lange (CdL) syndrome in mutation-negative CdL patients. Episignatures analysis of the in BAF complex components revealed novel functional protein interactions and common episignatures affecting homologous residues in highly conserved paralogous proteins (SMARCA2 M856V and SMARCA4 M866V). Finally, we also found sex-dependent episignatures in X-linked disorders. Implementation of episignature profiling is still in its early days, but with increasing utilization comes increasing awareness of the capacity of this methodology to help resolve the complex challenges of genetic diagnoses.

Original language	English
Article number	100309
Journal	Human Genetics and Genomics Advances
Volume	5
Issue number	3
Early online date	14 May 2024
DOIs	https://doi.org/10.1016/j.xhgg.2024.100309
Publication status	Published - 18 Jul 2024

Keywords

ARID1A
ARID1B
BAFopathy
Coffin-Siris syndrome
DNA methylation
SMARCA2
SMARCA4
SMARCB1
episignatures
neurodevelopmental disorders

Access to Document

10.1016/j.xhgg.2024.100309Licence: CC BY

Cite this

Trajkova, S., Kerkhof, J., Sebastiano, M. R., Pavinato, L., Ferrero, E., Giovenino, C., Carli, D., Di Gregorio, E., Marinoni, R., Mandrile, G., Palermo, F., Carestiato, S., Cardaropoli, S., Pullano, V., Rinninella, A., Giorgio, E., Pippucci, T., Dimartino, P., Rzasa, J., ... Brusco, A. (2024). DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity. Human Genetics and Genomics Advances, 5(3), Article 100309. https://doi.org/10.1016/j.xhgg.2024.100309

@article{84163720c2ef4382b8468147e8ac1305,

title = "DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity",

abstract = "Analysis of genomic DNA methylation by generating epigenetic signature profiles (episignatures) is increasingly being implemented in genetic diagnosis. Here we report our experience using episignature analysis to resolve both uncomplicated and complex cases of neurodevelopmental disorders (NDDs). We analyzed 97 NDDs divided into (1) a validation cohort of 59 patients with likely pathogenic/pathogenic variants characterized by a known episignature and (2) a test cohort of 38 patients harboring variants of unknown significance or unidentified variants. The expected episignature was obtained in most cases with likely pathogenic/pathogenic variants (53/59 [90\%]), a revealing exception being the overlapping profile of two SMARCB1 pathogenic variants with ARID1A/B:c.6200, confirmed by the overlapping clinical features. In the test cohort, five cases showed the expected episignature, including (1) novel pathogenic variants in ARID1B and BRWD3; (2) a deletion in ATRX causing MRXFH1 X-linked mental retardation; and (3) confirmed the clinical diagnosis of Cornelia de Lange (CdL) syndrome in mutation-negative CdL patients. Episignatures analysis of the in BAF complex components revealed novel functional protein interactions and common episignatures affecting homologous residues in highly conserved paralogous proteins (SMARCA2 M856V and SMARCA4 M866V). Finally, we also found sex-dependent episignatures in X-linked disorders. Implementation of episignature profiling is still in its early days, but with increasing utilization comes increasing awareness of the capacity of this methodology to help resolve the complex challenges of genetic diagnoses.",

keywords = "ARID1A, ARID1B, BAFopathy, Coffin-Siris syndrome, DNA methylation, SMARCA2, SMARCA4, SMARCB1, episignatures, neurodevelopmental disorders",

author = "Slavica Trajkova and Jennifer Kerkhof and Sebastiano, \{Matteo Rossi\} and Lisa Pavinato and Enza Ferrero and Chiara Giovenino and Diana Carli and \{Di Gregorio\}, Eleonora and Roberta Marinoni and Giorgia Mandrile and Flavia Palermo and Silvia Carestiato and Simona Cardaropoli and Verdiana Pullano and Antonina Rinninella and Elisa Giorgio and Tommaso Pippucci and Paola Dimartino and Jessica Rzasa and Kathleen Rooney and Haley McConkey and Aleksandar Petlichkovski and Barbara Pasini and Elena Sukarova-Angelovska and Campbell, \{Christopher M\} and Kay Metcalfe and Sarah Jenkinson and Siddharth Banka and Alessandro Mussa and Ferrero, \{Giovanni Battista\} and Bekim Sadikovic and Alfredo Brusco",

note = "Copyright {\textcopyright} 2024. Published by Elsevier Inc.",

year = "2024",

month = jul,

day = "18",

doi = "10.1016/j.xhgg.2024.100309",

language = "English",

volume = "5",

journal = "Human Genetics and Genomics Advances",

issn = "2666-2477",

publisher = "Elsevier BV",

number = "3",

}

Trajkova, S, Kerkhof, J, Sebastiano, MR, Pavinato, L, Ferrero, E, Giovenino, C, Carli, D, Di Gregorio, E, Marinoni, R, Mandrile, G, Palermo, F, Carestiato, S, Cardaropoli, S, Pullano, V, Rinninella, A, Giorgio, E, Pippucci, T, Dimartino, P, Rzasa, J, Rooney, K, McConkey, H, Petlichkovski, A, Pasini, B, Sukarova-Angelovska, E, Campbell, CM, Metcalfe, K, Jenkinson, S, Banka, S, Mussa, A, Ferrero, GB, Sadikovic, B & Brusco, A 2024, 'DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity', Human Genetics and Genomics Advances, vol. 5, no. 3, 100309. https://doi.org/10.1016/j.xhgg.2024.100309

TY - JOUR

T1 - DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity

AU - Trajkova, Slavica

AU - Kerkhof, Jennifer

AU - Sebastiano, Matteo Rossi

AU - Pavinato, Lisa

AU - Ferrero, Enza

AU - Giovenino, Chiara

AU - Carli, Diana

AU - Di Gregorio, Eleonora

AU - Marinoni, Roberta

AU - Mandrile, Giorgia

AU - Palermo, Flavia

AU - Carestiato, Silvia

AU - Cardaropoli, Simona

AU - Pullano, Verdiana

AU - Rinninella, Antonina

AU - Giorgio, Elisa

AU - Pippucci, Tommaso

AU - Dimartino, Paola

AU - Rzasa, Jessica

AU - Rooney, Kathleen

AU - McConkey, Haley

AU - Petlichkovski, Aleksandar

AU - Pasini, Barbara

AU - Sukarova-Angelovska, Elena

AU - Campbell, Christopher M

AU - Metcalfe, Kay

AU - Jenkinson, Sarah

AU - Banka, Siddharth

AU - Mussa, Alessandro

AU - Ferrero, Giovanni Battista

AU - Sadikovic, Bekim

AU - Brusco, Alfredo

PY - 2024/7/18

Y1 - 2024/7/18

N2 - Analysis of genomic DNA methylation by generating epigenetic signature profiles (episignatures) is increasingly being implemented in genetic diagnosis. Here we report our experience using episignature analysis to resolve both uncomplicated and complex cases of neurodevelopmental disorders (NDDs). We analyzed 97 NDDs divided into (1) a validation cohort of 59 patients with likely pathogenic/pathogenic variants characterized by a known episignature and (2) a test cohort of 38 patients harboring variants of unknown significance or unidentified variants. The expected episignature was obtained in most cases with likely pathogenic/pathogenic variants (53/59 [90%]), a revealing exception being the overlapping profile of two SMARCB1 pathogenic variants with ARID1A/B:c.6200, confirmed by the overlapping clinical features. In the test cohort, five cases showed the expected episignature, including (1) novel pathogenic variants in ARID1B and BRWD3; (2) a deletion in ATRX causing MRXFH1 X-linked mental retardation; and (3) confirmed the clinical diagnosis of Cornelia de Lange (CdL) syndrome in mutation-negative CdL patients. Episignatures analysis of the in BAF complex components revealed novel functional protein interactions and common episignatures affecting homologous residues in highly conserved paralogous proteins (SMARCA2 M856V and SMARCA4 M866V). Finally, we also found sex-dependent episignatures in X-linked disorders. Implementation of episignature profiling is still in its early days, but with increasing utilization comes increasing awareness of the capacity of this methodology to help resolve the complex challenges of genetic diagnoses.

AB - Analysis of genomic DNA methylation by generating epigenetic signature profiles (episignatures) is increasingly being implemented in genetic diagnosis. Here we report our experience using episignature analysis to resolve both uncomplicated and complex cases of neurodevelopmental disorders (NDDs). We analyzed 97 NDDs divided into (1) a validation cohort of 59 patients with likely pathogenic/pathogenic variants characterized by a known episignature and (2) a test cohort of 38 patients harboring variants of unknown significance or unidentified variants. The expected episignature was obtained in most cases with likely pathogenic/pathogenic variants (53/59 [90%]), a revealing exception being the overlapping profile of two SMARCB1 pathogenic variants with ARID1A/B:c.6200, confirmed by the overlapping clinical features. In the test cohort, five cases showed the expected episignature, including (1) novel pathogenic variants in ARID1B and BRWD3; (2) a deletion in ATRX causing MRXFH1 X-linked mental retardation; and (3) confirmed the clinical diagnosis of Cornelia de Lange (CdL) syndrome in mutation-negative CdL patients. Episignatures analysis of the in BAF complex components revealed novel functional protein interactions and common episignatures affecting homologous residues in highly conserved paralogous proteins (SMARCA2 M856V and SMARCA4 M866V). Finally, we also found sex-dependent episignatures in X-linked disorders. Implementation of episignature profiling is still in its early days, but with increasing utilization comes increasing awareness of the capacity of this methodology to help resolve the complex challenges of genetic diagnoses.

KW - ARID1A

KW - ARID1B

KW - BAFopathy

KW - Coffin-Siris syndrome

KW - DNA methylation

KW - SMARCA2

KW - SMARCA4

KW - SMARCB1

KW - episignatures

KW - neurodevelopmental disorders

UR - https://www.scopus.com/pages/publications/85195079453

UR - https://www.mendeley.com/catalogue/ec41d092-5e5b-39a3-a6de-cd3033d2a779/

U2 - 10.1016/j.xhgg.2024.100309

DO - 10.1016/j.xhgg.2024.100309

M3 - Article

C2 - 38751117

SN - 2666-2477

VL - 5

JO - Human Genetics and Genomics Advances

JF - Human Genetics and Genomics Advances

IS - 3

M1 - 100309

ER -

DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

NIHR Manchester Biomedical Research Centre

Cite this

DNA methylation analysis in patients with neurodevelopmental disorders improves variant interpretation and reveals complexity

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

Projects

NIHR Manchester Biomedical Research Centre

Cite this