The G protein-coupled receptor ligand apelin-13 ameliorates skeletal muscle atrophy induced by chronic kidney disease

Yuki Enoki; Tomoya Nagai; Yuna Hamamura; Sumika Osa; Hideaki Nakamura; Kazuaki Taguchi; Hiroshi Watanabe; Toru Maruyama; Kazuaki Matsumoto

doi:10.1002/jcsm.13159

The G protein-coupled receptor ligand apelin-13 ameliorates skeletal muscle atrophy induced by chronic kidney disease

J Cachexia Sarcopenia Muscle. 2023 Feb;14(1):553-564. doi: 10.1002/jcsm.13159. Epub 2022 Dec 23.

Authors

Yuki Enoki¹, Tomoya Nagai¹, Yuna Hamamura¹, Sumika Osa¹, Hideaki Nakamura², Kazuaki Taguchi¹, Hiroshi Watanabe³, Toru Maruyama³, Kazuaki Matsumoto¹

Affiliations

¹ Division of Pharmacodynamics, Keio University Faculty of Pharmacy, Tokyo, Japan.
² Faculty of Pharmaceutical Sciences, Sojo University, Kumamoto, Japan.
³ Department of Biopharmaceutics, Graduate School of Pharmaceutical Sciences, Kumamoto University, Kumamoto, Japan.

Abstract

Background: Targeting of the apelin-apelin receptor (Apj) system may serve as a useful therapeutic intervention for the management of chronic kidney disease (CKD)-induced skeletal muscle atrophy. We investigated the roles and efficacy of the apelin-Apj system in CKD-induced skeletal muscle atrophy.

Methods: The 5/6-nephrectomized mice were used as CKD models. AST-120, a charcoal adsorbent of uraemic toxins (8 w/w% in diet), or apelin (1 μmol/kg) was administered to CKD mice to investigate the mechanism and therapeutic potential of apelin on CKD-induced skeletal muscle atrophy. The effect of indoxyl sulfate, a uraemic toxin, or apelin on skeletal muscle atrophy was evaluated using mouse myoblast cells (C2C12 cells) in vitro.

Results: Skeletal muscle atrophy developed over time following nephrectomy at 12 weeks, as confirmed by a significant increase of atrogin-1 and myostatin mRNA expression in the gastrocnemius (GA) muscle and a decrease of lower limb skeletal muscle weight (P < 0.05, 0.01 and 0.05, respectively). Apelin expression in GA muscle was significantly decreased (P < 0.05) and elabela, another Apj endogenous ligand, tended to show a non-significant decrease at 12 weeks after nephrectomy. Administration of AST-120 inhibited the decline of muscle weight and increase of atrogin-1 and myostatin expression. Apelin and elabela expression was slightly improved by AST-120 administration but Apj expression was not, suggesting the involvement of uraemic toxins in endogenous Apj ligand expression. The administration of apelin at 1.0 μmol/kg for 4 weeks to CKD mice suppressed the increase of atrogin-1 and myostatin, increased apelin and Apj mRNA expression at 30 min after apelin administration and significantly ameliorated weight loss and a decrease of the cross-sectional area of hindlimb skeletal muscle.

Conclusions: This study demonstrated for the first time the association of the Apj endogenous ligand-uraemic toxin axis with skeletal muscle atrophy in CKD and the utility of therapeutic targeting of the apelin-Apj system.

Keywords: Apj; apelin; chronic kidney disease; elabela; skeletal muscle atrophy; uraemic toxin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apelin / metabolism
Apelin / pharmacology
Apelin / therapeutic use
Apelin Receptors / genetics
Apelin Receptors / metabolism
Ligands
Mice
Muscle, Skeletal / pathology
Muscular Atrophy / drug therapy
Muscular Atrophy / etiology
Muscular Atrophy / metabolism
Myostatin* / metabolism
RNA, Messenger / metabolism
Renal Insufficiency, Chronic* / drug therapy
Renal Insufficiency, Chronic* / etiology
Renal Insufficiency, Chronic* / metabolism
Uremic Toxins

Substances

apelin-13 peptide
Apelin
AST 120
Myostatin
Ligands
Uremic Toxins
Apelin Receptors
RNA, Messenger

Grants and funding

18K15069/JSPS KAKENHI