Downregulation by CNNM2 of ATP5MD expression in the 10q24.32 schizophrenia-associated locus involved in impaired ATP production and neurodevelopment.
Zhongju WangYongchang ZhuLinyan YeQiyang LiBo GuoHao ZhaoXiuqin BaoQiqi ZhuoTengfei YangZhaoqiang LiShufen LiBingtao HaoCunyou ZhaoPublished in: NPJ schizophrenia (2021)
Genome-wide association studies (GWAS) have accelerated the discovery of numerous genetic variants associated with schizophrenia. However, most risk variants show a small effect size (odds ratio (OR) <1.2), suggesting that more functional risk variants remain to be identified. Here, we employed region-based multi-marker analysis of genomic annotation (MAGMA) to identify additional risk loci containing variants with large OR value from Psychiatry Genomics Consortium (PGC2) schizophrenia GWAS data and then employed summary-data-based mendelian randomization (SMR) to prioritize schizophrenia susceptibility genes. The top-ranked susceptibility gene ATP5MD, encoding an ATP synthase membrane subunit, is observed to be downregulated in schizophrenia by the risk allele of CNNM2-rs1926032 in the schizophrenia-associated 10q24.32 locus. The Atp5md knockout (KO) in mice was associated with abnormal startle reflex and gait, and ATP5MD knockdown (KD) in human induced pluripotent stem cell-derived neurons disrupted the neural development and mitochondrial respiration and ATP production. Moreover, CNNM2-rs1926032 KO could induce downregulation of ATP5MD expression and disruptions of mitochondrial respiration and ATP production. This study constitutes an important mechanistic component that links schizophrenia-associated CNNM2 regions to disruption in energy adenosine system modulation and neuronal function by long-distance chromatin domain downregulation of ATP5MD. This pathogenic mechanism provides therapeutic implications for schizophrenia.
Keyphrases
- bipolar disorder
- copy number
- molecular dynamics
- poor prognosis
- genome wide
- signaling pathway
- oxidative stress
- endothelial cells
- cell proliferation
- gene expression
- dna methylation
- machine learning
- genome wide association study
- spinal cord
- brain injury
- single cell
- electronic health record
- big data
- insulin resistance
- functional connectivity
- resting state
- pluripotent stem cells
- binding protein
- cerebral ischemia