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首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Abuse Potential and Pharmacodynamic Characteristics of Oral and Intranasal Eluxadoline, a Mixed mu- and kappa-Opioid Receptor Agonist and delta-Opioid Receptor Antagonist
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Abuse Potential and Pharmacodynamic Characteristics of Oral and Intranasal Eluxadoline, a Mixed mu- and kappa-Opioid Receptor Agonist and delta-Opioid Receptor Antagonist

机译:口服和鼻内Eluxadoline,mu-和κ-阿片受体激动剂和δ-阿片受体拮抗剂的混合滥用潜能和药效学特征

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Drugs with mu-opioid receptor (OR) activity can be associated with abuse and misuse. The peripherally acting mixed mu-OR and kappa-OR agonist and delta-OR antagonist eluxadoline is approved in the United States for the treatment of irritable bowel syndrome with diarrhea. In two separate crossover studies, we evaluated the oral and intranasal abuse potential of eluxadoline versus placebo and the active control oxycodone. Healthy recreational opioid users received eluxadoline 100, 300, and 1000 mg, oxycodone 30 and 60 mg, and placebo (oral study), or eluxadoline 100 and 200 mg, oxycodone 15 and 30 mg, and placebos matched to eluxadoline and oxycodone (intranasal study). In the oral study, Drug Liking Visual Analog Scale (VAS) peak (maximum) effect (E-max) score (primary endpoint) was significantly greater with eluxadoline 300 and 1000 mg versus placebo, but scores were significantly lower versus oxycodone. Following intranasal insufflation of eluxadoline, Drug Liking VAS E-max scores were not statistically different versus placebo, and were significantly lower versus oxycodone. Across other subjective measures, eluxadoline was generally similar to or disliked versus placebo. Pupillometry indicated no or minimal central effects with oral and intranasal eluxadoline, respectively. Adverse events of euphoric mood were reported with oral and intranasal eluxadoline but at a far lower frequency versus oxycodone. These data demonstrate that eluxadoline has less abuse potential than oxycodone in recreational opioid users.
机译:具有阿片类药物受体(OR)活性的药物可能与滥用和滥用有关。外围作用的混合mu-OR和kappa-OR激动剂以及δ-OR拮抗剂eluxadoline在美国被批准用于治疗腹泻型肠易激综合症。在两项独立的交叉研究中,我们评估了依拉西多林与安慰剂和活性对照羟考酮的口服和鼻内滥用潜力。健康的娱乐性阿片类药物使用者接受eluxadoline 100、300和1000 mg,羟考酮30和60 mg以及安慰剂(口服研究),或eluxadoline 100和200 mg,羟考酮15和30 mg,安慰剂与eluxadoline和oxycodone匹配(鼻内研究) )。在口服研究中,依维多林300和1000 mg的药物喜欢视觉模拟量表(VAS)峰值(最大)作用(E-max)得分(主要终点)明显高于安慰剂,但与羟考酮相比得分明显更低。鼻腔注入氨甲酰胆碱后,喜欢药物的VAS E-max评分与安慰剂无统计学差异,与羟考酮相比显着降低。与其他主观指标相比,依拉西多林通常与安慰剂相似或不相似。眼压测定表明分别与口服和鼻内依拉西多林没有或仅有很少的中心作用。据报道,口服和鼻内依维拉多林引起欣快情绪的不良事件,但发生频率比羟考酮低得多。这些数据表明,在娱乐性阿片类药物使用者中,eluxadoline的滥用潜力低于羟考酮。

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