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GFRAL-expressing neurons suppress food intake via aversive pathways.


ABSTRACT: The TGFβ cytokine family member, GDF-15, reduces food intake and body weight and represents a potential treatment for obesity. Because the brainstem-restricted expression pattern of its receptor, GDNF Family Receptor α-like (GFRAL), presents an exciting opportunity to understand mechanisms of action for area postrema neurons in food intake; we generated GfralCre and conditional GfralCreERT mice to visualize and manipulate GFRAL neurons. We found infection or pathophysiologic states (rather than meal ingestion) stimulate GFRAL neurons. TRAP-Seq analysis of GFRAL neurons revealed their expression of a wide range of neurotransmitters and neuropeptides. Artificially activating GfralCre -expressing neurons inhibited feeding, decreased gastric emptying, and promoted a conditioned taste aversion (CTA). GFRAL neurons most strongly innervate the parabrachial nucleus (PBN), where they target CGRP-expressing (CGRPPBN) neurons. Silencing CGRPPBN neurons abrogated the aversive and anorexic effects of GDF-15. These findings suggest that GFRAL neurons link non-meal-associated pathophysiologic signals to suppress nutrient uptake and absorption.

SUBMITTER: Sabatini PV 

PROVIDER: S-EPMC7923658 | biostudies-literature | 2021 Feb

REPOSITORIES: biostudies-literature

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GFRAL-expressing neurons suppress food intake via aversive pathways.

Sabatini Paul V PV   Frikke-Schmidt Henriette H   Arthurs Joe J   Gordian Desiree D   Patel Anita A   Rupp Alan C AC   Adams Jessica M JM   Wang Jine J   Beck Jørgensen Sebastian S   Olson David P DP   Palmiter Richard D RD   Myers Martin G MG   Seeley Randy J RJ  

Proceedings of the National Academy of Sciences of the United States of America 20210201 8


The TGFβ cytokine family member, GDF-15, reduces food intake and body weight and represents a potential treatment for obesity. Because the brainstem-restricted expression pattern of its receptor, GDNF Family Receptor α-like (GFRAL), presents an exciting opportunity to understand mechanisms of action for area postrema neurons in food intake; we generated <i>Gfral</i><sup><i>Cre</i></sup> and conditional <i>Gfral</i><sup><i>CreERT</i></sup> mice to visualize and manipulate GFRAL neurons. We found  ...[more]

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