Towards precision medicine for anxiety disorders: objective assessment, risk prediction, pharmacogenomics, and repurposed drugs

dc.contributor.authorRoseberry, K.
dc.contributor.authorLe-Niculescu, H.
dc.contributor.authorLevey, D. F.
dc.contributor.authorBhagar, R.
dc.contributor.authorSoe, K.
dc.contributor.authorRogers, J.
dc.contributor.authorPalkowitz, S.
dc.contributor.authorPina, N.
dc.contributor.authorAnastasiadis, W. A.
dc.contributor.authorGill, S. S.
dc.contributor.authorKurian, S. M.
dc.contributor.authorShekhar, A.
dc.contributor.authorNiculescu, A. B.
dc.contributor.departmentPsychiatry, School of Medicine
dc.date.accessioned2024-04-18T13:07:08Z
dc.date.available2024-04-18T13:07:08Z
dc.date.issued2023
dc.description.abstractAnxiety disorders are increasingly prevalent, affect people's ability to do things, and decrease quality of life. Due to lack of objective tests, they are underdiagnosed and sub-optimally treated, resulting in adverse life events and/or addictions. We endeavored to discover blood biomarkers for anxiety, using a four-step approach. First, we used a longitudinal within-subject design in individuals with psychiatric disorders to discover blood gene expression changes between self-reported low anxiety and high anxiety states. Second, we prioritized the list of candidate biomarkers with a Convergent Functional Genomics approach using other evidence in the field. Third, we validated our top biomarkers from discovery and prioritization in an independent cohort of psychiatric subjects with clinically severe anxiety. Fourth, we tested these candidate biomarkers for clinical utility, i.e. ability to predict anxiety severity state, and future clinical worsening (hospitalizations with anxiety as a contributory cause), in another independent cohort of psychiatric subjects. We showed increased accuracy of individual biomarkers with a personalized approach, by gender and diagnosis, particularly in women. The biomarkers with the best overall evidence were GAD1, NTRK3, ADRA2A, FZD10, GRK4, and SLC6A4. Finally, we identified which of our biomarkers are targets of existing drugs (such as a valproate, omega-3 fatty acids, fluoxetine, lithium, sertraline, benzodiazepines, and ketamine), and thus can be used to match patients to medications and measure response to treatment. We also used our biomarker gene expression signature to identify drugs that could be repurposed for treating anxiety, such as estradiol, pirenperone, loperamide, and disopyramide. Given the detrimental impact of untreated anxiety, the current lack of objective measures to guide treatment, and the addiction potential of existing benzodiazepines-based anxiety medications, there is a urgent need for more precise and personalized approaches like the one we developed.
dc.eprint.versionFinal published version
dc.identifier.citationRoseberry K, Le-Niculescu H, Levey DF, et al. Towards precision medicine for anxiety disorders: objective assessment, risk prediction, pharmacogenomics, and repurposed drugs. Mol Psychiatry. 2023;28(7):2894-2912. doi:10.1038/s41380-023-01998-0
dc.identifier.urihttps://hdl.handle.net/1805/40112
dc.language.isoen_US
dc.publisherSpringer Nature
dc.relation.isversionof10.1038/s41380-023-01998-0
dc.relation.journalMolecular Psychiatry
dc.rightsAttribution 4.0 Internationalen
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.sourcePMC
dc.subjectGenetics
dc.subjectBiomarkers
dc.subjectAnxiety disorders
dc.subjectPharmacogenetics
dc.subjectBenzodiazepines
dc.subjectPrecision medicine
dc.subjectRisk assessment
dc.titleTowards precision medicine for anxiety disorders: objective assessment, risk prediction, pharmacogenomics, and repurposed drugs
dc.typeArticle
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