Blocking ActRIIB and Restoring Appetite Reverses Cachexia and Improves Survival in Mice with Lung Cancer

Overview

Journal Nat Commun

Specialty Biology

Date 2022 Aug 8

PMID 35941104

Authors

Andre Lima Queiroz

Ezequiel Dantas

Shakti Ramsamooj

Anirudh Murthy

Mujmmail Ahmed

Elizabeth R M Zunica

Roger J Liang

Jessica Murphy

Corey D Holman

Curtis J Bare

Gregory Ghahramani

Zhidan Wu

David E Cohen

John P Kirwan

Lewis C Cantley

Christopher L Axelrod

Marcus D Goncalves

Affiliations

Soon will be listed here.

Abstract

Cancer cachexia is a common, debilitating condition with limited therapeutic options. Using an established mouse model of lung cancer, we find that cachexia is characterized by reduced food intake, spontaneous activity, and energy expenditure accompanied by muscle metabolic dysfunction and atrophy. We identify Activin A as a purported driver of cachexia and treat with ActRIIB-Fc, a decoy ligand for TGF-β/activin family members, together with anamorelin (Ana), a ghrelin receptor agonist, to reverse muscle dysfunction and anorexia, respectively. Ana effectively increases food intake but only the combination of drugs increases lean mass, restores spontaneous activity, and improves overall survival. These beneficial effects are limited to female mice and are dependent on ovarian function. In agreement, high expression of Activin A in human lung adenocarcinoma correlates with unfavorable prognosis only in female patients, despite similar expression levels in both sexes. This study suggests that multimodal, sex-specific, therapies are needed to reverse cachexia.

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