Neuropeptide Y1 receptor expressing circuit from the central amygdala to lateral hypothalamus modulates binge‐like ethanol consumption in a sex‐dependent manner
Sophie C. Bendrath, Ashlyn Stone, Anne M. Dankert, Todd E. Thiele

TL;DR
This study explores how a specific brain circuit involving the central amygdala and lateral hypothalamus influences binge-like alcohol consumption differently in male and female mice.
Contribution
The study identifies a sex-dependent role of neuropeptide Y1 receptor signaling in a specific brain circuit in modulating binge-like ethanol consumption.
Findings
Chemogenetic inhibition of Y1R+ CeA-LH projections reduced binge-like ethanol drinking in male mice but not in females.
NPY overexpression in the CeA revealed behavioral effects and correlations between receptor mRNA expression and ethanol intake patterns.
Y1R expression levels varied with individual ethanol consumption, suggesting a neuroadaptive mechanism influenced by drinking patterns.
Abstract
Alcohol use disorder is characterized by maladaptive patterns of alcohol consumption, with emerging evidence suggesting that neuropeptide Y (NPY) signaling through Y1 and Y2 receptors (Y1R and Y2R) within the central amygdala (CeA) plays a critical role in modulating ethanol intake. The current experiments investigate the neural mechanisms underlying binge‐like ethanol drinking, focusing on the involvement of Y1R+ CeA‐to‐lateral hypothalamus (LH) projections, dynamic interactions between Y1R and Y2R within the CeA, and the impact of chronic ethanol exposure on Y1R protein expression. NPY1R‐ires‐cre mice received LH cannulation, were infused with cre‐dependent inhibitory (Gi) Designer Receptor Exclusively Activated by Designer Drug (DREADD) or control virus into the CeA, and went through drinking in the dark (DID). Other animals were treated intra‐CeA with an NPY overexpression vector…
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Taxonomy
TopicsRegulation of Appetite and Obesity · Neuropeptides and Animal Physiology · Neurotransmitter Receptor Influence on Behavior
