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首页> 外文期刊>European Journal of Pharmacology: An International Journal >dextro- and levo-morphine attenuate opioid delta and kappa receptor agonist produced analgesia in mu-opioid receptor knockout mice.
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dextro- and levo-morphine attenuate opioid delta and kappa receptor agonist produced analgesia in mu-opioid receptor knockout mice.

机译:右旋和左旋吗啡会减弱阿片类药物的含量,而κ受体激动剂可在mu阿片类受体敲除小鼠中产生镇痛作用。

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摘要

We have demonstrated that the antianalgesia induced by dextro-morphine and levo-morphine is not mediated by the stimulation of mu-opioid receptors in male CD-1 mice. We now report that the dextro-morphine and levo-morphine attenuated antinociception produced by delta-opioid receptor agonist deltorphin II and kappa-opioid receptor agonist U50,488H given spinally in the male mu-opioid receptor knockout mice. The tail-flick response was used for the antinociceptive test. Intrathecal injection of levo-morphine (3 nmol) markedly inhibited the tail-flick response in wild type, partially in heterozygous, but not in homozygous mu-opioid receptor knockout mice. Intrathecal pretreatment with dextro-morphine (33 fmol) or levo-morphine (0.3 nmol) for 45 min also attenuated levo-morphine-produced antinociception in wide type mice. Intrathecal pretreatment with dextro-morphine (33 fmol) or levo-morphine (0.3 nmol) for 45 min attenuated the tail-flick inhibition produced by deltorphin II (12.8 nmol) and U50,488H (123.3 nmol) in wide type, heterozygous and homozygous mu-opioid receptor knockout mice. The findings provide additional evidence that mu-opioid receptors are not involved in the antianalgesia induced by dextro-morphine and levo-morphine.
机译:我们已经证明,右旋吗啡和左吗啡诱导的镇痛作用不是由雄性CD-1小鼠中的μ阿片受体的刺激介导的。现在我们报道,雄性阿片类阿片受体敲除小鼠经脊髓给予δ-阿片受体激动剂deltorphin II和κ阿片受体激动剂U50,488H产生的右吗啡和左吗啡减毒镇痛作用。甩尾反应用于抗伤害感受试验。鞘内注射左吗啡(3 nmol)在野生型中明显抑制了甩尾反应,部分在杂合子中,但在纯合性阿片受体敲除小鼠中没有。鞘内用右旋吗啡(33 fmol)或左吗啡(0.3 nmol)预处理45分钟,在宽型小鼠中也减弱了左吗啡产生的镇痛作用。鞘内预处理使用右旋吗啡(33 fmol)或左吗啡(0.3 nmol)持续45分钟,可减轻deltorphin II(12.8 nmol)和U50,488H(123.3 nmol)在宽型,杂合和纯合中产生的甩尾抑制作用mu阿片受体敲除小鼠。该发现提供了进一步的证据,表明阿片类药物受体不参与右旋吗啡和左吗啡诱导的抗痛觉过敏。

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