Epigenetic mechanisms, like those involving DNA methylation, are thought to mediate the relationship between chronic cocaine dependence and molecular changes in addiction-related neurocircuitry, but have been understudied in human brain. We initially used reduced representation bisulfite sequencing (RRBS) to generate a methylome-wide profile of cocaine dependence in human post-mortem caudate tissue. We focused on the Iroquois Homeobox A (IRXA) gene cluster, where hypomethylation in exon 3 of IRX2 in neuronal nuclei was associated with cocaine dependence. We replicated this finding in an independent cohort and found similar results in the dorsal striatum from cocaine self-administering mice. Using epigenome editing and 3C assays, we demonstrated a causal relationship between methylation within the IRX2 gene body, CTCF protein binding, three-dimensional (3D) chromatin interaction, and gene expression. Together, these findings suggest that cocaine-related hypomethylation of IRX2 contributes to the development and maintenance of cocaine dependence through alterations in 3D chromatin structure in the caudate nucleus.
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| http://dx.doi.org/10.1038/s41380-020-00909-x | DOI Listing |
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Article Synopsis
- Impulsivity and behavioral inhibition are linked to substance misuse, especially cocaine use disorder, with variations based on cocaine use history and dependence levels.
- Rats in this study self-administered cocaine under different access conditions: one group had extended access (6 hours) while the other had short access (1 hour), to evaluate behavioral inhibition.
- Results showed that rats with extended cocaine access demonstrated significantly impaired behavioral inhibition compared to both their baseline performance and the short access group, suggesting that heavy cocaine use negatively affects the ability to inhibit future use.
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