Germline pathogenic variants in HNRNPU are associated with alterations in blood methylome

Author:

Balasubramanian Meena1,Lee Sunwoo2,Ochoa Eguzkine2,Badura-Stronka Magdalena3,Donnelly Deirdre4,Lederer Damien5,Lynch Sally,Gardham Alice,Morton Jenny,Stewart Helen6,Docquier France2,Rodger Fay2,Martin Jose2,Toribio Ana2,Maher Eamonn2ORCID,Balasubramanian Meena1

Affiliation:

1. Sheffield Children's NHS Foundation Trust

2. University of Cambridge

3. Poznan University of Medical Sciences

4. Belfast Health and Social Care Trust

5. Centre for Human Genetics, Institute of Pathology and Genetics

6. Oxford University Hospitals NHS Trust

Abstract

Abstract HNRNPU encodes a multifunctional RNA-binding protein that plays critical roles in regulating pre-mRNA splicing, mRNA stability, and translation. Aberrant expression and dysregulation of HNRNPU have been implicated in various human diseases, including cancers and neurological disorders. We applied a next generation sequencing based assay (EPIC-NGS) to investigate genome-wide methylation profiling for > 2M CpGs for 7 individuals with a neurodevelopmental disorder associated with HNRNPU germline pathogenic loss-of-function variants. Compared to healthy individuals, 227 HNRNPU-associated differentially methylated positions were detected. Both hyper- and hypomethylation alterations were identified but the former predominated. The identification of a methylation episignature for HNRNPU-associated neurodevelopmental disorder (NDD) implicates HNPRNPU-related chromatin alterations in the aetiopathogenesis of this disorder and suggests that episignature profiling should have clinical utility as a predictor for the pathogenicity of HNRNPU variants of uncertain significance. The detection of a methylation episignaure for HNRNPU-associated NDD is consistent with a recent report of a methylation episignature for HNRNPK-associated NDD.

Publisher

Research Square Platform LLC

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