The common adverse effect of centrally-injected mu-opioid receptor (mu-OR) agonists is pruritus. This study was conducted using mice to examine whether different subtypes of mu-OR would be responsible for pruritus and analgesia. Intracisternal injections of morphine and morphine-6beta-glucronide (M6G), but not M3G, produced an antinociceptive effect. Morphine, but neither M6G nor M3G, induced facial scratching, a pruritus-related response. Facial scratching following morphine was not affected by the mu(1)-OR antagonist naloxonazine at doses that inhibited the antinociceptive effects. The results suggest that different subtype and/or splice variants of mu-OR are separately involved in pruritus and antinociception of opioids.

译文

集中注射mu-阿片受体 (mu-OR) 激动剂的常见不良反应是瘙痒。这项研究是使用小鼠进行的,以检查mu-OR的不同亚型是否会引起瘙痒和镇痛。脑内注射吗啡和morphine-6beta-glucronide (M6G),而不是M3G,产生抗伤害感受作用。吗啡,但M6G和M3G都不会引起面部抓挠,这是一种瘙痒相关的反应。吗啡后的面部抓挠不受mu(1) 或拮抗剂纳洛酮嗪抑制抗伤害感受作用的影响。结果表明,mu-or的不同亚型和/或剪接变体分别参与阿片类药物的瘙痒和抗伤害感受。

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