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Biomarker discovery in attention deficit hyperactivity disorder: RNA sequencing of whole blood in discordant twin and case-controlled cohorts. | LitMetric

AI Article Synopsis

  • Researchers explored the link between genetic markers and RNA gene expression in ADHD, utilizing advanced RNA sequencing methods on blood samples from twins and adolescents.* -
  • By comparing data from discordant twins and case-controlled ADHD subjects, they identified specific RNA markers that are potential indicators of ADHD.* -
  • The findings highlight genes previously linked to ADHD and suggest that combining DNA, RNA, and metabolic data could lead to new diagnostic tools and treatments.*

Article Abstract

Background: A variety of DNA-based methods have been applied to identify genetic markers of attention deficit hyperactivity disorder (ADHD), but the connection to RNA-based gene expression has not been fully exploited.

Methods: Using well defined cohorts of discordant, monozygotic twins from the Michigan State University Twin Registry, and case-controlled ADHD cases in adolescents, the present studies utilized advanced single molecule RNA sequencing to identify expressed changes in whole blood RNA in ADHD. Multiple analytical strategies were employed to narrow differentially expressed RNA targets to a small set of potential biomarkers of ADHD.

Results: RNA markers common to both the discordant twin study and case-controlled subjects further narrowed the putative targets, some of which had been previously associated with ADHD at the DNA level. The potential role of several differentially expressed genes, including ABCB5, RGS2, GAK, GIT1 and 3 members of the galactose metabolism pathway (GALE, GALT, GALK1) are substantiated by prior associations to ADHD and by established mechanistic connections to molecular pathways relevant to ADHD and behavioral control.

Conclusions: The convergence of DNA, RNA, and metabolic data suggests these may be promising targets for diagnostics and therapeutics in ADHD.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7594430PMC
http://dx.doi.org/10.1186/s12920-020-00808-8DOI Listing

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