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Long-term effects of ghrelin and ghrelin receptor agonists on energy balance in rats

机译:生长激素释放肽和生长素释放肽受体激动剂对大鼠能量平衡的长期影响

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摘要

Ghrelin, an endogenous ligand of the growth hormone secretagogue receptor (GHS-R), is the only circulating agent to powerfully promote a positive energy balance. Such action is mediated predominantly by central nervous system pathways controlling food intake, energy expenditure, and nutrient partitioning. The ghrelin pathway may therefore offer therapeutic potential for the treatment of catabolic states. However, the potency of the endogenous hormone ghrelin is limited due to a short half-life and the fragility of its bioactivity ensuring acylation at serine 3. Therefore, we tested the metabolic effects of two recently generated GHS-R agonists, BIM-28125 and BIM-28131, compared with ghrelin. All agents were administered continuously for 1 mo in doses of 50 and 500 nmol·kg−1·day−1 using implanted subcutaneous minipumps in rats. High-dose treatment with single agonists or ghrelin increased body weight gain by promoting fat mass, whereas BIM-28131 was the only one also increasing lean mass significantly. Food intake increased during treatment with BIM-28131 or ghrelin, whereas no effects on energy expenditure were detected. With the lower dose, only BIM-28131 had a significant effect on body weight. This also held true when the compound was administered by subcutaneous injection three times/day. No symptoms or signs of undesired effects were observed in any of the studies or treated groups. These results characterize BIM-28131 as a promising GHS-R agonist with an attractive action profile for the treatment of catabolic disease states such as cachexia.
机译:生长激素促分泌素受体(GHS-R)的内源性配体Ghrelin是唯一能强烈促进正能量平衡的循环剂。这种作用主要由控制食物摄入,能量消耗和营养分配的中枢神经系统途径介导。 ghrelin途径因此可提供治疗分解代谢状态的治疗潜力。但是,由于半衰期短以及其生物活性的脆弱性(确保丝氨酸3上有酰化作用),内源性生长激素释放肽的效力受到限制。因此,我们测试了两种最近产生的GHS-R激动剂BIM-28125和BIM-28131与Ghrelin相比。使用植入的皮下微型泵在大鼠中以50和500 nmol·kg-1·day-1的剂量连续给药1个月。用单种激动剂或生长素释放肽进行大剂量治疗可通过促进脂肪量增加体重增加,而BIM-28131是唯一也显着增加瘦肉量的人。在用BIM-28131或生长素释放肽治疗期间,食物摄入量增加,但未发现对能量消耗的影响。在较低剂量下,只有BIM-28131对体重有显着影响。当该化合物通过皮下注射每天3次给药时,也是如此。在任何研究或治疗组中均未观察到不良症状或体征。这些结果将BIM-28131表征为一种有前途的GHS-R激动剂,具有有吸引力的作用谱,可用于治疗分解代谢性疾病,例如恶病质。

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