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Role of DNA Methylation in Mediating Genetic Risk of Psychiatric Disorders

期刊

FRONTIERS IN PSYCHIATRY
卷 12, 期 -, 页码 -

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fpsyt.2021.596821

关键词

epigenetic regulation; DNA methylation; mQTL; CpG-SNP; GWAS; psychiatric disorder

资金

  1. Lundbeck Foundation (Denmark)
  2. H2020 Program [667302]

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Psychiatric disorders are a common cause of disability worldwide, with research focusing on genetic risk variants like SNPs and their impact on DNA methylation. Understanding how these variants contribute to the pathophysiology of psychiatric disorders is essential for future research and treatment strategies.
Psychiatric disorders are common, complex, and heritable conditions estimated to be the leading cause of disability worldwide. The last decade of research in genomics of psychiatry, performed by multinational, and multicenter collaborative efforts on hundreds of thousands of mental disorder cases and controls, provided invaluable insight into the genetic risk variants of these conditions. With increasing cohort sizes, more risk variants are predicted to be identified in the near future, but there appears to be a knowledge gap in understanding how these variants contribute to the pathophysiology of psychiatric disorders. Majority of the identified common risk single-nucleotide polymorphisms (SNPs) are non-coding but are enriched in regulatory regions of the genome. It is therefore of great interest to study the impact of identified psychiatric disorders' risk SNPs on DNA methylation, the best studied epigenetic modification, playing a pivotal role in the regulation of transcriptomic processes, brain development, and functioning. This work outlines the mechanisms through which risk SNPs can impact DNA methylation levels and provides a summary of current evidence on the role of DNA methylation in mediating the genetic risk of psychiatric disorders.

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