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首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Pharmacological characterization of ATPM ((-)-3-aminothiazolo(5,4-b)-N-cyclopropylmethylmorphinan hydrochloride), a novel mixed kappa-agonist and mu-agonist/-antagonist that attenuates morphine antinociceptive tolerance and heroin self-administration
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Pharmacological characterization of ATPM ((-)-3-aminothiazolo(5,4-b)-N-cyclopropylmethylmorphinan hydrochloride), a novel mixed kappa-agonist and mu-agonist/-antagonist that attenuates morphine antinociceptive tolerance and heroin self-administration

机译:ATPM((-)-3-氨基噻唑(5,4-b)-N-环丙基甲基吗啡盐酸盐)的药理学表征

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摘要

ATPM [(-)-3-amino-thiazolo[5,4-b]-N-cyclopropylmethylmorphinan hydrochloride] was found to have mixed kappa- and mu-opioid activity and identified to act as a full kappa-agonist and a partial mu-agonist by in vitro binding assays. The present study was undertaken to characterize its in vivo effects on morphine antinociceptive tolerance in mice and heroin self-administration in rats. ATPM was demonstrated to yield more potent antinociceptive effects than (-)U50,488H (trans-3,4-dichloro-N-methyl-N-[2-(1-pyrrolidinyl)cyclohexyl]benzeneacetamide). It was further found that the antinociceptive effects of ATPM were mediated by kappa- and mu-, but not delta-opioid, receptors. In addition to its agonist profile on the mu-receptor, ATPM also acted as a mu-antagonist, as measured by its inhibition of morphine-induced antinociception. It is more important that ATPM had a greater ratio of the ED(50) value of sedation to that of antinociception than (-)U50,488 (11.8 versus 3.7), indicative of a less sedative effectthan (-)U50,488H. In addition, ATPM showed less potential to develop antinociceptive tolerance relative to (-)U50,488H and morphine. Moreover, it dose-dependently inhibited morphine-induced antinociceptive tolerance. Furthermore, it was found that chronic treatment of rats for 8 consecutive days with ATPM (0.5 mg/kg s.c.) produced sustained decreases in heroin self-administration. (-)U50,488H (2 mg/kg s.c.) also produced similar inhibitory effect. Taken together, our findings demonstrated that ATPM, a novel mixed kappa-agonist and mu-agonist/-antagonist, could inhibit morphine-induced antinociceptive tolerance, with less potential to develop tolerance and reduce heroin self-administration with less sedative effect. kappa-Agonists with some mu-activity appear to offer some advantages over selective kappa-agonists for the treatment of heroin abuse.
机译:发现ATPM [(-)-3-氨基噻唑并[5,4-b] -N-环丙基甲基吗啡喃盐酸盐]具有混合的κ和μ阿片样物质活性,并被鉴定为具有完整的κ激动剂和部分μ -受体激动剂的体外结合试验。进行本研究以表征其对小鼠吗啡抗伤害感受耐受和大鼠海洛因自我给药的体内作用。与(-)U50,488H(反式-3,4-二氯-N-甲基-N- [2-(1-吡咯烷基)环己基]苯乙酰胺)相比,ATPM具有更强的镇痛作用。进一步发现,ATPM的抗伤害感受作用是由κ受体和μ受体而非δ阿片受体介导的。通过在吗啡诱导的抗伤害感受中的抑制作用,ATPM除了在mu受体上具有激动剂特性外,还可以充当mu拮抗剂。更为重要的是,与(-)U50,488相比,ATPM的镇静ED(50)值与抗伤害感受的比率更大(11.8比3.7),表明镇静作用比(-)U50,488H小。此外,相对于(-)U50,488H和吗啡,ATPM显示出较小的抗伤害感受性的潜力。此外,它剂量依赖性地抑制吗啡诱导的镇痛耐受性。此外,发现用ATPM(0.5mg / kg s.c.)连续8天对大鼠进行长期治疗会导致海洛因自我给药的持续减少。 (-)U50,488H(2 mg / kg s.c.)也产生了相似的抑制作用。两者合计,我们的研究结果表明,新型的混合kappa激动剂和mu激动剂/拮抗剂ATPM可以抑制吗啡诱导的抗伤害感受性耐受性,产生耐受性的可能性较小,减少海洛因自我给药的镇静作用较小。在治疗海洛因滥用方面,具有一定mu活性的kappa激动剂似乎比选择性kappa激动剂更具优势。

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