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

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Zengbing Lu , Man P. Ngan , Julia Y.H Liu , Lingqing Yang , Longlong Tu , Sze Wa Chan , Claudio Giuliano , Emanuela Lovati , Claudio Pietra , John A. Rudd
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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 [IC50]=14.0 µM) and 54.4 % (IC50=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.

生长激素分泌受体 1a 激动剂 anamorelin 和 ipamorelin 可抑制顺铂引起的雪貂体重下降:anamorelin 还可通过中枢机制发挥止吐作用。
本研究探讨了胃泌素模拟物(即阿那莫瑞林和伊帕莫瑞林)是否能减轻顺铂诱导的雪貂急性期和延迟期的体重下降和进食抑制。阿那莫瑞林与伊帕莫瑞林比较了阿那莫瑞林抑制电场刺激(EFS)诱导的离体雪貂回肠收缩的潜力。在其他实验中,雪貂在顺铂(5 毫克/千克,静脉注射)前 30 秒腹腔注射阿那莫瑞林(1-3 毫克/千克)、伊帕莫瑞林(1-3 毫克/千克)或载体,然后每隔 24 小时注射一次,并记录其行为长达 72 小时。每 24 小时测量一次食物和水的消耗量。脑室内给药后还评估了阿那莫瑞林(10微克)的效果。阿那莫瑞林和伊帕莫瑞林对EFS诱导的离体回肠收缩的抑制率分别为94.4%(半最大抑制浓度[IC50]=14.0µM)和54.4%(IC50=11.7µM)。静脉注射这两种化合物对顺铂诱导的急性或延迟性呕吐均无任何影响,但在延迟期的最后一天(48-72小时),这两种化合物都能抑制顺铂诱导的相关体重减轻约24%。脑室内注射阿那莫林(10微克)可将顺铂诱导的急性呕吐减少60%,但不影响延迟性呕吐。此外,阿那莫瑞林还能使急性期的食物和水消耗量增加约20%-40%,但对延迟期没有影响,并能使延迟期顺铂诱导的相关体重减轻23%。总之,静脉注射阿那莫瑞林和伊帕莫瑞林对缓解顺铂诱导的延迟期体重减轻有好处,而且这些效果在中枢注射阿那莫瑞林时也能看到。脑室内给药而非腹膜内给药后,阿莫瑞林可抑制顺铂诱发的急性呕吐,这表明脑穿透对其止吐作用机制非常重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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