The growth hormone secretagogue receptor 1a agonists, anamorelin and ipamorelin, inhibit cisplatin-induced weight loss in ferrets: Anamorelin also exhibits anti-emetic effects via a central mechanism.
Lu. Zengbing Z; Ngan. Man P MP; Liu. Julia Y H JYH; Yang. Lingqing L; Tu. Longlong L; Chan. Sze Wa SW; Giuliano. Claudio C; Lovati. Emanuela E; Pietra. Claudio C; Rudd. John A JA
Key Findings
- Both ipamorelin (1‑3 mg/kg) and anamorelin (1‑3 mg/kg) reduced cisplatin‑induced weight loss by ~24 % during the delayed phase in ferrets
- Anamorelin was more effective than ipamorelin at relaxing intestinal muscle (94 % vs 54 % inhibition)
- Only central (intracerebroventricular) administration of anamorelin cut acute vomiting by ~60 %; peripheral injection had no anti‑emetic effect
Practical Outcomes
- These results suggest ipamorelin might help preserve body weight under severe catabolic stress, but there’s no evidence it boosts appetite or prevents nausea in healthy people. The anti‑vomit benefit seen with anamorelin requires brain access, which typical peripheral dosing doesn’t provide. Enthusiasts should view these findings as early animal data, not a ready‑to‑use protocol for humans.
Summary
In a ferret study, the growth‑hormone‑releasing peptides ipamorelin and anamorelin helped lessen weight loss caused by the chemotherapy drug cisplatin, but only when given during the later (delayed) phase of the illness. Only anamorelin, when injected directly into the brain, reduced vomiting right after the drug, showing that it needs to reach the brain to work as an anti‑nausea agent. The usual peripheral injection of either peptide didn’t stop vomiting.
Abstract
This study investigated whether ghrelin mimetics, namely anamorelin and ipamorelin, can alleviate weight loss and inhibition of feeding observed during acute and delayed phases of cisplatin-induced emesis in ferrets. The potential of anamorelin to inhibit electrical field stimulation (EFS)-induced contractions of isolated ferret ileum was compared with ipamorelin. In other experiments, ferrets were administered anamorelin (1-3 mg/kg), ipamorelin (1-3 mg/kg), or vehicle intraperitoneally (i.p.) 30 s before cisplatin (5 mg/kg, i.p.) and then every 24 h, and their behaviour was recorded for up to 72 h. Food and water consumption was measured every 24 h. The effect of anamorelin (10 µg) was also assessed following intracerebroventricular administration. Anamorelin and ipamorelin inhibited EFS-induced contractions of isolated ileum by 94.4 % (half-maximal inhibitory concentration [IC<sub>50</sub>]=14.0 µM) and 54.4 % (IC<sub>50</sub>=11.7 µM), respectively. Neither of compounds administered i.p. had any effect on cisplatin-induced acute or delayed emesis, but both inhibited associated cisplatin-induced weight loss on the last day of delayed phase (48-72 h) by approximately 24 %. Anamorelin (10 µg) administered intracerebroventricularly reduced cisplatin-induced acute emesis by 60 % but did not affect delayed emesis. It also improved food and water consumption by approximately 20 %-40 % during acute phase, but not delayed phase, and reduced associated cisplatin-induced weight loss during delayed phase by ∼23 %. In conclusion, anamorelin and ipamorelin administered i.p. had beneficial effects in alleviating cisplatin-induced weight loss during delayed phase, and these effects were seen when centrally administered anamorelin. Anamorelin inhibited cisplatin-induced acute emesis following intracerebroventricular but not intraperitoneal administration, suggesting that brain penetration is important for its anti-emetic mechanism of action.
Study Information
pubmed
2024
2024-07-21T00:00:00.000Z
10.1016/j.physbeh.2024.114644
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