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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Pharmacological characterization of naloxegol: In vitro and in vivo studies
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Pharmacological characterization of naloxegol: In vitro and in vivo studies

机译:纳洛昔尔的药理特征:体外和体内研究

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Opioid-induced constipation is the most prevalent adverse effect of opioid drugs. Peripherally acting mu opioid receptor antagonists (PAMORAs), including naloxegol, are indicated for the treatment of opioid-induced constipation. The aim of this study was the in vitro and in vivo pharmacological characterization of naloxegol in comparison with naloxone. In vitro experiments were performed to measure calcium mobilization in cells coexpressing opioid receptors and chimeric G proteins and mu receptor interaction with G protein and beta-arrestin 2 using bioluminescence resonance energy transfer. In vivo experiments were performed in mice to measure pain threshold using the tail withdrawal assay and colonic transit using the bead expulsion assay. In vitro, naloxegol behaved as a selective and competitive mu receptor antagonist similarly to naloxone, being 3-10-fold less potent. In vivo, naloxone was effective in blocking fentanyl actions when given subcutaneously (sc), but not per os (po). In contrast, naloxegol elicited very similar effects with sc or po administration counteracting in a dose dependent manner the constipating effects of fentanyl without interfering with the fentanyl mediated analgesia. Thus, a useful PAMORA action could be obtained with naloxegol both after po and sc administration.
机译:阿片类药物引起的便秘是阿片类药物最常见的不良反应。外周作用的mu阿片受体拮抗剂(PAMORA),包括纳洛酮,用于治疗阿片诱导的便秘。本研究的目的是比较纳洛酮与纳洛酮在体外和体内的药理特性。体外实验采用生物发光共振能量转移法测量了共表达阿片受体和嵌合G蛋白的细胞中的钙动员,以及mu受体与G蛋白和β-阻遏蛋白2的相互作用。在小鼠身上进行了体内实验,以使用尾部撤回试验测量痛阈,并使用珠粒排出试验测量结肠转运。在体外,纳洛酮与纳洛酮类似,是一种选择性和竞争性的mu受体拮抗剂,效力低3-10倍。在体内,纳洛酮在皮下给药(sc)时能有效阻断芬太尼的作用,但在经皮给药(po)时不能。相比之下,纳洛酮与sc或po给药产生非常相似的效果,以剂量依赖性的方式抵消芬太尼的便秘效应,而不干扰芬太尼介导的镇痛。因此,在po和sc给药后,纳洛酮都可以发挥有益的帕莫拉作用。

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