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促黑素细胞激素4受体(MC4R)激动剂setmelanotide与雄性小鼠高碳酸血症化学敏感性改善及体重减轻有关。

The MC4R agonist, setmelanotide, is associated with an improvement in hypercapnic chemosensitivity and weight loss in male mice.

作者信息

Rivera Athena, Framnes-DeBoer Sarah N, Arble Deanna M

机构信息

Department of Biological Sciences, Marquette University, WI, USA.

Department of Biological Sciences, Marquette University, WI, USA.

出版信息

Respir Physiol Neurobiol. 2025 Feb-Mar;332:104370. doi: 10.1016/j.resp.2024.104370. Epub 2024 Nov 13.

DOI:10.1016/j.resp.2024.104370
PMID:39542230
Abstract

Obesity increases the risk of respiratory diseases that reduce respiratory chemosensitivity, such as Obesity Hypoventilation Syndrome and sleep apnea. Recent evidence suggests that obesity-related changes in the brain, including alterations in melanocortin signaling via the melanocortin-4 receptor (MC4R), may underly altered chemosensitivity. Setmelanotide, an MC4R agonist, causes weight loss in both humans and animal models. However, it is unknown the extent to which setmelanotide affects respiratory chemosensitivity independent of body weight loss. The present study uses diet-induced obese, male C57bl/6 J mice to determine the extent to which acute setmelanotide treatment affects the hypercapnic ventilatory response (HCVR). We find that ten days of daily setmelanotide treatment at 1 mg/kg, but not 0.2 mg/kg, is sufficient to cause weight loss and increase HCVR. In a separate group of animals, we find that we can emulate setmelanotide's effect on weight loss by restricting daily calories to match the hypophagia triggered by setmelanotide. These pair-fed animals exhibit improvements in HCVR similar to those who receive setmelanotide. We conclude that acute treatment with setmelanotide is as effective as weight loss at improving respiratory hypercapnic chemosensitivity.

摘要

肥胖会增加降低呼吸化学敏感性的呼吸道疾病风险,如肥胖低通气综合征和睡眠呼吸暂停。最近的证据表明,大脑中与肥胖相关的变化,包括通过黑皮质素-4受体(MC4R)的黑皮质素信号改变,可能是化学敏感性改变的基础。Setmelanotide是一种MC4R激动剂,可导致人类和动物模型体重减轻。然而,尚不清楚Setmelanotide在多大程度上独立于体重减轻而影响呼吸化学敏感性。本研究使用饮食诱导肥胖的雄性C57bl/6 J小鼠来确定急性Setmelanotide治疗对高碳酸通气反应(HCVR)的影响程度。我们发现,每天以1 mg/kg而非0.2 mg/kg的剂量使用Setmelanotide治疗十天,足以导致体重减轻并增加HCVR。在另一组动物中,我们发现通过限制每日热量摄入以匹配Setmelanotide引发的食欲减退,我们可以模拟Setmelanotide对体重减轻的影响。这些配对喂养的动物在HCVR方面的改善与接受Setmelanotide的动物相似。我们得出结论,Setmelanotide的急性治疗在改善呼吸高碳酸化学敏感性方面与体重减轻一样有效。

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The Molecular Circadian Clock of Phox2b-expressing Cells Drives Daily Variation of the Hypoxic but Not Hypercapnic Ventilatory Response in Mice.表达 Phox2b 的细胞的分子生物钟驱动小鼠缺氧但非高碳酸通气反应的日变化。
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