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. 2025 Feb 25;44(2):115332.
doi: 10.1016/j.celrep.2025.115332. Epub 2025 Feb 15.

A multi-omics and cell type-specific characterization of the ventral striatum in human cocaine use disorder

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A multi-omics and cell type-specific characterization of the ventral striatum in human cocaine use disorder

Eric Zillich et al. Cell Rep. .

Abstract

Epigenome, transcriptome, and proteome analyses of postmortem brains have revealed initial molecular insights into cocaine use disorder (CUD). However, the inter-relationship between these omics and the contribution of individual cell types remains largely unknown. We present an in-depth analysis of molecular changes in the ventral striatum in CUD at multi-omics and single-cell resolution. Integrative multi-omics analyses of microRNA sequencing (microRNA-seq), RNA sequencing (RNA-seq), and proteomics datasets in 41 individuals and single-nuclei RNA-seq in a subset of 16 individuals revealed conserved deregulation of metabolic pathways, oxidative phosphorylation, and glutamatergic signaling. Cell type-specific analyses identified inverse metabolic pathway deregulation patterns in glial and neuronal cells, notably in astrocytes and medium-spiny neurons (MSNs). Characterizing astrocyte-neuron crosstalk revealed altered glutamatergic and cell-cell adhesion signaling in CUD. By applying a comprehensive multi-omics analytical framework, our study provides novel insights into CUD-associated molecular changes in the ventral striatum highlighting the perturbation of astrocytes, MSNs, and their crosstalk in CUD.

Keywords: CP: Neuroscience; addiction; cocaine use disorder; miRNA-seq; multi-omics; postmortem brain tissue; proteomics; single-nuclei RNA-seq.

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Conflict of interest statement

Declaration of interests The authors declare that there are no competing interests.

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