1. Academic Validation
  2. Functional coupling between MC4R and Kir7.1 contributes to clozapine-induced hyperphagia

Functional coupling between MC4R and Kir7.1 contributes to clozapine-induced hyperphagia

  • bioRxiv. 2024 Jun 8:2024.06.07.597973. doi: 10.1101/2024.06.07.597973.
Li Li Ciria C Hernandez Luis E Gimenez Baijie Xu Naima S Dahir Swati Shari G Birnbaum Roger D Cone Chen Liu
Abstract

Most antipsychotic drugs (APDs) induce hyperphagia and weight gain. However, the neural mechanisms are poorly understood, partly due to challenges replicating their metabolic effects in rodents. Here, we report a new mouse model that recapitulates overeating induced by clozapine, a widely prescribed APD. Our study shows that clozapine boosts food intake by inhibiting melanocortin 4 receptor (MC4R) expressing neurons in the paraventricular nucleus of the hypothalamus. Interestingly, neither clozapine nor risperidone, another commonly used APD, affects receptor-ligand binding or the canonical Gαs signaling of MC4R. Instead, they inhibit neuronal activity by enhancing the coupling between MC4R and Kir7.1, leading to the open state of the inwardly rectifying Potassium Channel. Deletion of Kir7.1 in Mc4r-Cre neurons prevents clozapine-induced weight gain, while treatment with a selective Kir7.1 blocker mitigates overeating in clozapine-fed mice. Our findings unveil a molecular pathway underlying the effect of APDs on feeding behavior and suggest its potential as a therapeutic target.

Figures
Products