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Outpatient opiate detoxification treatment with buprenorphine. Preliminary investigation.丁丙诺啡门诊阿片类药物脱毒治疗。初步调查。
Eur Addict Res. 1998 Dec;4(4):198-202. doi: 10.1159/000018953.
2
Motivational properties of buprenorphine as assessed by place and taste conditioning in rats.通过大鼠的位置和味觉条件反射评估丁丙诺啡的动机特性。
Psychopharmacology (Berl). 1997 Mar;130(2):104-8. doi: 10.1007/s002130050216.
3
Kinetics of respiratory depression in rats induced by buprenorphine and its metabolite, norbuprenorphine.丁丙诺啡及其代谢产物去甲丁丙诺啡诱导大鼠呼吸抑制的动力学
J Pharmacol Exp Ther. 1997 Apr;281(1):428-33.
4
Pharmacological characterization of buprenorphine, a mixed agonist-antagonist with kappa 3 analgesia.丁丙诺啡的药理学特性,一种具有κ3镇痛作用的混合激动剂-拮抗剂。
Brain Res. 1997 Jan 2;744(1):41-6. doi: 10.1016/s0006-8993(96)01069-4.
5
Buprenorphine exerts its antinociceptive activity via mu 1-opioid receptors.丁丙诺啡通过μ1阿片受体发挥其镇痛活性。
Life Sci. 1995 Mar 3;56(15):PL285-90. doi: 10.1016/0024-3205(95)00078-x.
6
The effects of chronic morphine on the generalization of buprenorphine stimulus control: an assessment of kappa antagonist activity.慢性吗啡对丁丙诺啡刺激控制泛化的影响:κ拮抗剂活性评估
Pharmacol Biochem Behav. 1995 Dec;52(4):779-87. doi: 10.1016/0091-3057(95)00180-5.
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Consumption of buprenorphine and other drugs among heroin addicts under ambulatory treatment: results from cross-sectional studies in 1988 and 1990.门诊治疗的海洛因成瘾者中丁丙诺啡及其他药物的使用情况:1988年和1990年横断面研究结果
Addiction. 1993 Oct;88(10):1341-9. doi: 10.1111/j.1360-0443.1993.tb02020.x.
8
Dissociation of buprenorphine-induced locomotor sensitization and conditioned place preference in rats.丁丙诺啡诱导的大鼠运动敏化与条件性位置偏爱之间的分离
Pharmacol Biochem Behav. 1994 Sep;49(1):241-5. doi: 10.1016/0091-3057(94)90484-7.
9
Buprenorphine self-administration by rhesus monkey.恒河猴的丁丙诺啡自我给药
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Ligand: a versatile computerized approach for characterization of ligand-binding systems.配体:一种用于表征配体结合系统的通用计算机化方法。
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HS-599:一种新型长效阿片类镇痛药不会在大鼠中诱发位置偏爱。

HS-599: a novel long acting opioid analgesic does not induce place-preference in rats.

作者信息

Lattanzi R, Negri L, Giannini E, Schmidhammer H, Schutz J, Improta G

机构信息

Department of Human Physiology and Pharmacology, University 'La Sapienza', P.le Aldo Moro, 5, I-00185 Rome, Italy.

出版信息

Br J Pharmacol. 2001 Sep;134(2):441-7. doi: 10.1038/sj.bjp.0704280.

DOI:10.1038/sj.bjp.0704280
PMID:11564664
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1572965/
Abstract
  1. When administered subcutaneously HS-599, a new didehydroderivative of buprenorphine (18,19-dehydrobuprenorphine), produced a long-lasting antinociceptive response in rats. Its potency exceeded twice that of buprenorphine. In the tail-flick test it acted as a full agonist but in the plantar test only as a partial agonist. Whereas the mu-opioid antagonists naloxone and naltrexone antagonized HS-599 antinociception the delta-opioid antagonist naltrindole and the kappa-opioid antagonist nor-binaltorphimine did not. 2. Unlike buprenorphine and morphine, HS-599 never induced conditioned place-preference in rats. 3. In radioligand binding assays, compared with buprenorphine HS-599 had 3 fold higher mu-opioid receptor affinity but lower delta- and kappa-opioid receptor affinity. 4. In isolated guinea-pig ileum preparations, HS-599 only partially inhibited the electrically-stimulated contraction, acting as a partial opioid agonist. When tested against the mu-opioid receptor agonist dermorphin, it behaved as a non-equilibrium antagonist. Conversely, in mouse vas deferens (rich in delta-opioid receptors) and rabbit vas deferens preparations (rich in kappa-opioid receptors) HS-599 acted as a pure equilibrium antagonist, shifting the log-concentration-response curves of the delta-opioid agonist deltorphin I and the kappa-opioid agonist U-69593 to the right. 5. In conclusion, HS-599 is a novel buprenorphine derivative with higher affinity, selectivity and potency than the parent compound, for mu-opioid receptors. It produces intense and long-lasting antinociception and does not induce place-preference in rats.
摘要
  1. 皮下注射丁丙诺啡的一种新的双脱氢衍生物HS - 599(18,19 - 脱氢丁丙诺啡)时,在大鼠中产生了持久的抗伤害感受反应。其效力超过丁丙诺啡两倍以上。在甩尾试验中它表现为完全激动剂,但在足底试验中仅为部分激动剂。μ - 阿片受体拮抗剂纳洛酮和纳曲酮可拮抗HS - 599的抗伤害感受作用,而δ - 阿片受体拮抗剂纳曲吲哚和κ - 阿片受体拮抗剂去甲二氢吗啡酮则不能。2. 与丁丙诺啡和吗啡不同,HS - 599从未在大鼠中诱导出条件性位置偏爱。3. 在放射性配体结合试验中,与丁丙诺啡相比,HS - 599对μ - 阿片受体的亲和力高3倍,但对δ - 和κ - 阿片受体的亲和力较低。4. 在离体豚鼠回肠制备物中,HS - 599仅部分抑制电刺激收缩,表现为部分阿片激动剂。当与μ - 阿片受体激动剂德莫啡肽进行测试时,它表现为非平衡拮抗剂。相反,在富含δ - 阿片受体的小鼠输精管和富含κ - 阿片受体的兔输精管制备物中,HS - 599表现为纯平衡拮抗剂,将δ - 阿片激动剂德尔托啡肽I和κ - 阿片激动剂U - 69593的对数浓度 - 反应曲线向右移动。5. 总之,HS - 599是一种新型丁丙诺啡衍生物,对μ - 阿片受体的亲和力、选择性和效力均高于母体化合物。它能产生强烈且持久的抗伤害感受作用,并且不会在大鼠中诱导位置偏爱。