SEPTO-HYPOTHALAMIC REGULATION OF BINGE-LIKE ALCOHOL CONSUMPTION BY THE NOCICEPTIN SYSTEM

Septo-hypothalamic regulation of binge-like alcohol consumption by the nociceptin system

Septo-hypothalamic regulation of binge-like alcohol consumption by the nociceptin system

Blog Article

Summary: High-intensity alcohol drinking during binge episodes contributes to the socioeconomic burden created by alcohol use disorders (AUDs), and nociceptin receptor (NOP) antagonists have emerged as a promising intervention.To better understand the contribution of the NOP Ringette - Cages system to binge drinking, we found that nociceptin-containing neurons of the lateral septum (LSPnoc) displayed increased excitability during withdrawal from binge-like alcohol drinking.LSPnoc activation promoted active avoidance and potentiated binge-like drinking behavior, whereas silencing of this population reduced alcohol drinking.

LSPnoc form robust monosynaptic inputs locally within the LS and genetic deletion of NOP or microinjection of a NOP antagonist into the LS decreased NA@8 alcohol intake.LSPnoc also project to the lateral hypothalamus and supramammillary nucleus of the hypothalamus, and genetic deletion of NOP from each site reduced alcohol drinking.Together, these findings implicate the septo-hypothalamic nociceptin system in excessive alcohol consumption and support NOP antagonist development for the treatment of AUD.

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