米芬太尼可拮抗吗啡诱导的小鼠脾脏自然杀伤细胞活性抑制。
Mirfentanil antagonizes morphine-induced suppression of splenic NK activity in mice.
作者信息
Carr D J, Brockunier L L, Scott M, Bagley J R, France C P
机构信息
Department of Microbiology, Immunology, Parasitology, Louisiana State University Medical Center, New Orleans 70112-1393, USA.
出版信息
Immunopharmacology. 1996 Aug;34(1):9-16. doi: 10.1016/0162-3109(95)00051-8.
Mirfentanil [N-(2-pyrazinyl)-N-(1-phenethyl-4-piperidinyl)-2-furamide] was studied for its antinociceptive and immunomodulatory effects in mice Mirfentanil (1.0-32.0 mg/kg) increased tail-flick latency to a thermal stimulus and this effect was antagonized (94 +/- 2%) by naltrexone (10.0 mg/kg). Unlike naltrexone, the delta opioid selective antagonist naltrindole (20.0 mg/kg) had no effect on mirfentanil-induced analgesia. In a dose-dependent fashion, the mu-selective antagonists beta-funaltrexamine (1.0-40.0 mg/kg) and naloxonazine (1.0-35.0 mg/kg) blocked mirfentanil (10.0 mg/kg)-induced analgesia up to 75% of the maximum analgesic effect. Norbinaltorphimine (10.0 mg/kg) partially blocked (35%) the maximum analgesic effect following mirfentanil (10.0 mg/kg) administration. Single doses of mirfentanil (0.1-32.0 mg/kg) had no effect on splenic NK activity. However, preadministration of mirfentanil (1.0-10.0 mg/kg) blocked morphine-induced suppression of splenic NK activity. Collectively, the results suggest that mirfentanil is a novel opioid that induces antinociception predominately through mu opioid receptors but, unlike morphine or fentanyl, does not suppress splenic NK activity.
研究了米尔芬太尼[N-(2-吡嗪基)-N-(1-苯乙基-4-哌啶基)-2-呋喃甲酰胺]对小鼠的镇痛和免疫调节作用。米尔芬太尼(1.0 - 32.0毫克/千克)可增加对热刺激的甩尾潜伏期,且这种作用可被纳曲酮(10.0毫克/千克)拮抗(94±2%)。与纳曲酮不同,δ阿片受体选择性拮抗剂纳曲吲哚(20.0毫克/千克)对米尔芬太尼诱导的镇痛无影响。μ选择性拮抗剂β-芬太尼丁胺(1.0 - 40.0毫克/千克)和纳洛嗪(1.0 - 35.0毫克/千克)以剂量依赖方式阻断米尔芬太尼(10.0毫克/千克)诱导的镇痛,最高可达最大镇痛效果的75%。去甲丙氧芬(10.0毫克/千克)部分阻断(35%)米尔芬太尼(10.0毫克/千克)给药后的最大镇痛效果。单剂量的米尔芬太尼(0.1 - 32.0毫克/千克)对脾脏自然杀伤细胞活性无影响。然而,预先给予米尔芬太尼(1.0 - 10.0毫克/千克)可阻断吗啡诱导的脾脏自然杀伤细胞活性抑制。总体而言,结果表明米尔芬太尼是一种新型阿片类药物,主要通过μ阿片受体诱导镇痛,但与吗啡或芬太尼不同,不抑制脾脏自然杀伤细胞活性。
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