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Dryad

Good vs poor responder RNAseq transcriptome profiles in DBA/2J mice

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Nov 23, 2020 version files 38.67 MB

Abstract

Major depressive disorder is the most prevalent mental illness worldwide, still its pharmacological treatment is limited by various challenges, such as the large heterogeneity in treatment response and the lack of insight into the neurobiological pathways underlying this phenomenon. To decode the molecular mechanisms shaping antidepressant response and to distinguish those from general paroxetine effects, we used a previously established approach targeting extremes (i.e. good vs. poor responder mice). Transcriptome profiling on micro-dissected DG granule cells as well as on peripheral blood samples was performed to i) reveal celltype specific changes in paroxetine-induced gene expression (paroxetine vs. vehicle) and ii) to identify molecular signatures of treatment response within a cohort of paroxetine-treated animals. In this datasheet, we provide the mapped and norm-counted RNAseq results of our experiments in an user-friendly excel file.