Reciprocal Control of Obesity and Anxiety-depressive Disorder Via a GABA and Serotonin Neural Circuit

Overview

Journal Mol Psychiatry

Specialties Molecular Biology
Psychiatry

Date 2021 Mar 26

PMID 33767348

Citations 34

Authors

Guobin Xia

Yong Han

Fantao Meng

Yanlin He

Dollada Srisai

Monica Farias

Minghao Dang

Richard D Palmiter

Yong Xu

Qi Wu

Affiliations

Soon will be listed here.

Abstract

The high comorbidity between obesity and mental disorders, such as depression and anxiety, often exacerbates metabolic and neurological symptoms significantly. However, neural mechanisms that underlie reciprocal control of feeding and mental states are largely elusive. Here we report that melanocortin 4 receptor (MC4R) neurons located in the dorsal bed nucleus of the stria terminus (dBNST) engage in the regulation of mentally associated weight gain by receiving GABAergic projections from hypothalamic AgRP neurons onto α5-containing GABA receptors and serotonergic afferents onto 5-HT receptors. Chronic treatment with a high-fat diet (HFD) significantly blunts the hyperexcitability of AgRP neurons in response to not only hunger but also anxiety and depression-like stimuli. Such HFD-mediated desensitization reduces GABAergic outputs from AgRP neurons to downstream MC4R neurons, resulting in severe mental dysregulation. Genetic enhancement of the GABAR-α5 or suppression of the 5-HTR within the MC4R neurons not only abolishes HFD-induced anxiety and depression but also robustly reduces body weight by suppression of food intake. To gain further translational insights, we revealed that combined treatment of zonisamide (enhancing the GABAR-α5 signaling) and granisetron (a selective 5-HTR antagonist) alleviates mental dysfunction and yields a robust reversal of diet-induced obesity by reducing total calorie intake and altering food preference towards a healthy low-fat diet. Our results unveil a neural mechanism for reciprocal control of appetite and mental states, which culminates in a novel zonisamide-granisetron cocktail therapy for potential tackling the psychosis-obesity comorbidity.

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