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Overriding the blockade of antinociceptive actions of opioids in rats treated with extended-release naltrexone.

机译:克服了用缓释纳曲酮治疗的大鼠中阿片类药物的镇痛作用的阻断作用。

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A monthly extended-release formulation of the opioid antagonist naltrexone (XR-NTX) is approved for treatment of alcohol dependence. There is little research regarding overriding chronic (>21 days) competitive opioid receptor blockade with opioids for acute pain. Using the hot plate test after XR-NTX or placebo microsphere administration, rats were treated with an opioid analgesic to determine the dose required to produce the maximum response latency (MRL; 60 s). Rats were later treated with the same opioid to determine any potential effects on respiration rate or locomotor activity. In naive rats, 15 mg/kg morphine, 0.1 mg/kg fentanyl and 8 mg/kg hydrocodone produced MRL. In XR-NTX treated rats, morphine produced 36% and 46% MRL at 90 mg/kg on days 4 and 19 and 96% MRL at 45 mg/kg on day 39. Fentanyl produced 100% MRL at 2.0 mg/kg on days 4 and 19 and at 0.5 mg/kg on day 39. Hydrocodone (80 mg/kg) produced 69%, 80% and 100% MRL on days 4, 19 and 39. Compared to placebo, these doses did not further depress respiration or alter locomotor activity. Thus, opioid receptor blockade with XR-NTX can be overcome in rats with higher doses of opioids without further affecting respiration or locomotor activity.
机译:阿片拮抗剂纳曲酮(XR-NTX)的每月延长释放制剂被批准用于治疗酒精依赖症。很少有关于用阿片类药物替代慢性(超过21天)竞争性阿片受体阻滞剂治疗急性疼痛的研究。使用XR-NTX或安慰剂微球给药后的热板测试,用阿片类镇痛药治疗大鼠,以确定产生最大反应潜伏期(MRL; 60 s)所需的剂量。随后用相同的阿片类药物治疗大鼠,以确定对呼吸速率或运动能力的任何潜在影响。在幼稚大鼠中,15 mg / kg吗啡,0.1 mg / kg芬太尼和8 mg / kg氢可酮产生了最大残留限量。在XR-NTX处理的​​大鼠中,吗啡在第4天和第19天分别以90 mg / kg的剂量产生36%和46%的MRL,在第39天产生45 mg / kg的96%的MRL。芬太尼第几天产生的2.0 mg / kg的100%MRL 4和19,第39天的剂量为0.5 mg / kg。氢可酮(80 mg / kg)在第4、19和39天产生69%,80%和100%的最大残留限量。与安慰剂相比,这些剂量并未进一步抑制呼吸或改变运动活动。因此,在较高剂量的阿片类药物中,可以克服XR-NTX对阿片类药物受体的阻滞作用,而不会进一步影响呼吸或运动能力。

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