Genome-wide DNA methylation risk scores for schizophrenia derived from blood and brain tissues further explain the genetic risk in patients stratified by polygenic risk scores for schizophrenia and bipolar disorder-Reference-Cited by-同舟云学术

Genome-wide DNA methylation risk scores for schizophrenia derived from blood and brain tissues further explain the genetic risk in patients stratified by polygenic risk scores for schizophrenia and bipolar disorder

Published:2024-01 Issue:1 Volume:27 Page:e300936
ISSN:2755-9734
Container-title:BMJ Mental Health
language:en
Short-container-title:BMJ Ment Health

Author:

Ohi Kazutaka^ORCID,Shimada Mihoko,Soda Midori,Nishizawa Daisuke,Fujikane Daisuke,Takai Kentaro,Kuramitsu Ayumi,Muto Yukimasa,Sugiyama Shunsuke,Hasegawa Junko,Kitaichi Kiyoyuki,Ikeda Kazutaka,Shioiri Toshiki

Abstract

BackgroundGenetic and environmental factors contribute to the pathogenesis of schizophrenia (SZ) and bipolar disorder (BD). Among genetic risk groups stratified by combinations of Polygenic Risk Score (PRS) deciles for SZ, BD and SZ versus BD, genetic SZ risk groups had high SZ risk and prominent cognitive impairments. Furthermore, epigenetic alterations are implicated in these disorders. However, it was unclear whether DNA Methylation Risk Scores (MRSs) for SZ risk derived from blood and brain tissues were associated with SZ risk, particularly the PRS-stratified genetic SZ risk group.MethodsEpigenome-wide association studies (EWASs) of SZ risk in whole blood were preliminarily conducted between 66 SZ patients and 30 healthy controls (HCs) and among genetic risk groups (individuals with low genetic risk for SZ and BD in HCs (n=30) and in SZ patients (n=11), genetic BD risk in SZ patients (n=25) and genetic SZ risk in SZ patients (n=30)) stratified by combinations of PRSs for SZ, BD and SZ versus BD. Next, differences in MRSs based on independent EWASs of SZ risk in whole blood, postmortem frontal cortex (FC) and superior temporal gyrus (STG) were investigated among our case‒control and PRS-stratified genetic risk status groups.ResultsAmong case‒control and genetic risk status groups, 33 and 351 genome-wide significant differentially methylated positions (DMPs) associated with SZ were identified, respectively, many of which were hypermethylated. Compared with the low genetic risk in HCs group, the genetic SZ risk in SZ group had 39 genome-wide significant DMPs, while the genetic BD risk in SZ group had only six genome-wide significant DMPs. The MRSs for SZ risk derived from whole blood, FC and STG were higher in our SZ patients than in HCs in whole blood and were particularly higher in the genetic SZ risk in SZ group than in the low genetic risk in HCs and genetic BD risk in SZ groups. Conversely, the MRSs for SZ risk based on our whole-blood EWASs among genetic risk groups were also associated with SZ in the FC and STG. There were no correlations between the MRSs and PRSs.ConclusionsThese findings suggest that the MRS is a potential genetic marker in understanding SZ, particularly in patients with a genetic SZ risk.

Publisher

BMJ

Reference57 articles.

1. A comprehensive nationwide study of the incidence rate and lifetime risk for treated mental disorders;Pedersen;JAMA Psychiatry,2014

2. Prevalence and Correlates of Bipolar Spectrum Disorder in the World Mental Health Survey Initiative

3. Schizophrenia as a Complex Trait

4. Family, twin, and adoption studies of bipolar disorder;Smoller;American J of Med Genetics Pt C,2003

5. Mapping Genomic Loci Implicates genes and synaptic biology in schizophrenia;Trubetskoy;Nature,2022