"Genomic DNA Methylation Signatures Enable Concurrent Diagnosis and Cli" by Erfan Aref-Eshghi, David I Rodenhiser et al.

Paediatrics Publications

Title

Genomic DNA Methylation Signatures Enable Concurrent Diagnosis and Clinical Genetic Variant Classification in Neurodevelopmental Syndromes

Authors

Erfan Aref-Eshghi, Western University
David I Rodenhiser, Western University
Laila C Schenkel, Western University
Hanxin Lin, Western University
Cindy Skinner, Greenwood Genetics Center
Peter Ainsworth, Western University
Guillaume Paré, McMaster University
Rebecca L Hood, University of Ottawa
Dennis E Bulman, University of Ottawa
Kristin D Kernohan, University of Ottawa
Care4Rare Canada Consortium
Kym M Boycott, University of Ottawa
Philippe M Campeau, University of Montreal
Charles Schwartz, Greenwood Genetics Center
Bekim Sadikovic, Western University

Document Type

Article

Publication Date

1-4-2018

Journal

American Journal of Human Genetics

Volume

102

Issue

First Page

156

Last Page

174

URL with Digital Object Identifier

https://doi.org/10.1016/j.ajhg.2017.12.008

Abstract

Pediatric developmental syndromes present with systemic, complex, and often overlapping clinical features that are not infrequently a consequence of Mendelian inheritance of mutations in genes involved in DNA methylation, establishment of histone modifications, and chromatin remodeling (the "epigenetic machinery"). The mechanistic cross-talk between histone modification and DNA methylation suggests that these syndromes might be expected to display specific DNA methylation signatures that are a reflection of those primary errors associated with chromatin dysregulation. Given the interrelated functions of these chromatin regulatory proteins, we sought to identify DNA methylation epi-signatures that could provide syndrome-specific biomarkers to complement standard clinical diagnostics. In the present study, we examined peripheral blood samples from a large cohort of individuals encompassing 14 Mendelian disorders displaying mutations in the genes encoding proteins of the epigenetic machinery. We demonstrated that specific but partially overlapping DNA methylation signatures are associated with many of these conditions. The degree of overlap among these epi-signatures is minimal, further suggesting that, consistent with the initial event, the downstream changes are unique to every syndrome. In addition, by combining these epi-signatures, we have demonstrated that a machine learning tool can be built to concurrently screen for multiple syndromes with high sensitivity and specificity, and we highlight the utility of this tool in solving ambiguous case subjects presenting with variants of unknown significance, along with its ability to generate accurate predictions for subjects presenting with the overlapping clinical and molecular features associated with the disruption of the epigenetic machinery.

Link to Full Text

COinS

Paediatrics Publications

Title

Authors

Document Type

Publication Date

Journal

Volume

Issue

First Page

Last Page

URL with Digital Object Identifier

Abstract

Links

Browse

Author Corner

Paediatrics Publications

Title

Authors

Document Type

Publication Date

Journal

Volume

Issue

First Page

Last Page

URL with Digital Object Identifier

Abstract

Share

Links

Browse

Author Corner