EXT418, a novel long‐acting ghrelin, mitigates Lewis lung carcinoma induced cachexia in mice

Author:

Kerr Haiming L.12ORCID,Krumm Kora12,Lee Ian (In‐gi)12,Anderson Barbara12,Christiani Anthony12,Strait Lena12,Breckheimer Beatrice A.12,Irwin Brynn12,Jiang Alice (Siyi)12,Rybachok Artur12,Chen Amanda12,Caeiro Lucas12,Dacek Elizabeth12,Hall Daniel B.3,Kostyla Caroline H.34,Hales Laura M.3,Soliman Tarik M.3,Garcia Jose M.12ORCID

Affiliation:

1. Geriatric Research, Education and Clinical Center Veterans Affairs Puget Sound Health Care System Seattle Washington USA

2. Department of Medicine, Division of Gerontology and Geriatric Medicine University of Washington School of Medicine Washington Seattle USA

3. Extend Biosciences, Inc. St. Newton Massachusetts USA

4. Atalanta Therapeutics Boston Massachusetts USA

Abstract

AbstractBackgroundGhrelin is a potential therapy for cachexia due to its orexigenic properties and anabolic effects on muscle and fat. However, its clinical use is limited by the short half‐life of active (acylated) ghrelin (~11 min in humans). EXT418 is a novel long‐acting, constitutively active ghrelin analog created by covalently linking it to a vitamin D derivative. Here, we evaluated the effects and mechanisms of action of EXT418 on Lewis lung carcinoma (LLC)‐induced cachexia in mice.MethodsMale C57BL/6J mice (5‐ to 7‐month‐old) were implanted with 1 × 106 heat‐killed (HK) or live LLC cells. When the tumour was palpable, mice were injected with vehicle (T + V) or EXT418 daily (T + 418 Daily, 0.25 mg/kg/day) or every other day (T + 418 EOD, 0.5 mg/kg/EOD) for up to 14 days, whereas HK‐treated mice were given vehicle (HK + V). Subsets of T + 418 Daily or EOD‐treated mice were pair‐fed to the T + V group. Body composition and grip strength were evaluated before tumour implantation and at the end of the experiment. Molecular markers were probed in muscles upon termination.ResultsIn tumour‐bearing mice, administration of EXT418 daily or EOD partially prevented weight loss (T + V vs. T + 418 Daily, P = 0.030; and vs. T + 418 EOD, P = 0.020). Similar effects were observed in whole body fat and lean body mass. Grip strength in tumour‐bearing mice was improved by EXT418 daily (P = 0.010) or EOD (P = 0.008) administration compared with vehicle‐treated mice. These effects of EXT418 on weight and grip strength were partially independent of food intake. EXT418 daily administration also improved type IIA (P = 0.015), IIB (P = 0.037) and IIX (P = 0.050) fibre cross‐sectional area (CSA) in tibialis anterior (TA) and EXT418 EOD improved CSA of IIB fibres in red gastrocnemius (GAS; P = 0.005). In skeletal muscles, tumour‐induced increases in atrogenes Fbxo32 and Trim63 were ameliorated by EXT418 treatments (TA and GAS/plantaris, PL), which were independent of food intake. EXT418 administration decreased expression of the mitophagy marker Bnip3 (GAS/PL; P ≤ 0.010). Similar effects of EXT418 EOD were observed in p62 (GAS/PL; P = 0.039). In addition, EXT418 treatments ameliorated the tumour‐induced elevation in muscle Il6 transcript levels (TA and GAS/PL), independently of food intake. Il‐6 transcript levels in adipose tissue and circulating IL‐10 were elevated in response to the tumour but these increases were not significant with EXT418 administration. Tumour mass was not altered by EXT418.ConclusionsEXT418 mitigates LLC‐induced cachexia by attenuating skeletal muscle inflammation, proteolysis, and mitophagy, without affecting tumour mass and partially independent of food intake.

Funder

U.S. Department of Veterans Affairs

Common Fund

Congressionally Directed Medical Research Programs

Nutrition Obesity Research Center, University of North Carolina

Publisher

Wiley

Subject

Physiology (medical),Orthopedics and Sports Medicine

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