Yoburn B C, Shah S, Chan K, Duttaroy A, Davis T
Department of Pharmaceutical Sciences, College of Pharmacy and Allied Health Professions, St. John's University, Queens, NY 11439, USA.
Pharmacol Biochem Behav. 1995 Jun-Jul;51(2-3):535-9. doi: 10.1016/0091-3057(94)00375-s.
The effect of chronic opioid antagonist treatment on the analgesic potency of six opioid agonists was compared to changes in opioid receptor density and the selectivity of each agonist for mu (DAMGO), delta (DPDPE) and kappa (U69,593) opioid receptors. Mice were implanted SC with a 15-mg naltrexone or placebo pellet for 8 days. The pellets were removed and 24 h later, mice were sacrificed and binding studies were conducted, or mice were tested in analgesia (tail-flick) dose-response studies. All six analgesics acted as full agonists for both placebo and naltrexone-treated mice. Naltrexone increased the analgesic potency of methadone, etorphine, fentanyl, meperidine, and oxycodone by 1.9-3.2-fold. The analgesic potency of propoxyphene was not increased significantly (1.3-fold). In saturation binding studies in brain homogenate, naltrexone increased the Bmax of mu, delta, and kappa opioid receptors by 86, 43, and 33%, respectively, without altering Kd. Competition binding studies for each receptor type were conducted in brains from untreated mice, and KIs were determined for each agonist. All agonists had greatest selectivity toward mu compared with delta and kappa receptors. There did not appear to be an obvious relationship between receptor selectivity and the magnitude of supersensitivity. These studies indicate that supersensitivity occurs for a broad range of opioid analgesics following chronic opioid antagonist treatment in the mouse. However, the selectivity of these agonists for mu, delta, and kappa receptors does not appear to correlate with differences in supersensitivity.
将慢性阿片类拮抗剂治疗对六种阿片类激动剂镇痛效力的影响与阿片受体密度的变化以及每种激动剂对μ(DAMGO)、δ(DPDPE)和κ(U69,593)阿片受体的选择性进行了比较。给小鼠皮下植入15毫克纳曲酮或安慰剂药丸,持续8天。取出药丸,24小时后处死小鼠并进行结合研究,或者对小鼠进行镇痛(甩尾)剂量反应研究。对于安慰剂和纳曲酮处理的小鼠,所有六种镇痛药均表现为完全激动剂。纳曲酮使美沙酮、埃托啡、芬太尼、哌替啶和羟考酮的镇痛效力提高了1.9至3.2倍。丙氧芬的镇痛效力没有显著提高(1.3倍)。在脑匀浆的饱和结合研究中,纳曲酮使μ、δ和κ阿片受体的Bmax分别增加了86%、43%和33%,而不改变Kd。在未处理小鼠的脑中对每种受体类型进行竞争结合研究,并确定每种激动剂的抑制常数(KI)。与δ和κ受体相比,所有激动剂对μ受体的选择性最高。受体选择性与超敏反应的程度之间似乎没有明显的关系。这些研究表明,在小鼠中进行慢性阿片类拮抗剂治疗后,多种阿片类镇痛药都会出现超敏反应。然而,这些激动剂对μ、δ和κ受体的选择性似乎与超敏反应的差异无关。
