current
May 22nd, 2024 at 5:25pm
Overview
Abstract
Midbrain dopamine neurons (DNs) respond to a first exposure to addictive drugs and play key roles in chronic drug usage (1-3) . As the synaptic and transcriptional changes that follow an acute cocaine exposure are mostly resolved within a few days (4,5) , the molecular changes that encode the long-term cellular memory of the exposure within DNs remain unknown. To investigate whether a single cocaine exposure induces long-term changes in the 3D genome structure of DNs, we applied Genome Architecture Mapping and single nucleus transcriptomic analyses in the mouse midbrain. We found extensive rewiring of 3D genome architecture at 24 hours past exposure which remains or worsens by 14 days, outlasting transcriptional responses. The cocaine-induced chromatin rewiring occurs at all genomic scales and affects genes with major roles in cocaine-induced synaptic changes. A single cocaine exposure triggers extensive long-lasting changes in chromatin condensation in post-synaptic and post-transcriptional regulatory genes, for example the unfolding of Rbfox1 which becomes most prominent 14 days post exposure. Finally, structurally remodeled genes are most expressed in a specific DN sub-type characterized by low expression of the dopamine auto-receptor Drd2 , a key feature of highly cocaine-sensitive cells. These results reveal an important role for long-lasting 3D genome remodelling in the cellular memory of a single cocaine exposure, providing new hypotheses for understanding the inception of drug addiction and 3D genome plasticity.
Authors
Szabo D • Franke V • Bianco S • Batiuk MY • Paul EJ • Kukalev A • Pfisterer UG • Irastorza-Azcarate I • Chiariello AM • Demharter S • Zea-Redondo L • Lopez-Atalaya JP • Nicodemi M • Akalin A • Khodosevich K • Ungless MA • Winick-Ng W • Pombo A
Link
Journal
bioRxiv : the preprint server for biology
PMID:38766140
Published
May 12th, 2024