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首页> 外文期刊>Clinical Pharmacology and Therapeutics >ADL 8-2698, a trans-3,4-dimethyl-4-(3-hydroxyphenyl) piperidine, prevents gastrointestinal effects of intravenous morphine without affecting analgesia.
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ADL 8-2698, a trans-3,4-dimethyl-4-(3-hydroxyphenyl) piperidine, prevents gastrointestinal effects of intravenous morphine without affecting analgesia.

机译:ADL 8-2698,一种反式3,4-二甲基-4-(3-羟苯基)哌啶,可预防静脉内吗啡的胃肠道作用,而不会影响镇痛作用。

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摘要

ADL-8-2698 is a novel peripherally restricted opioid antagonist that may selectively prevent opioid-induced gastrointestinal effects without reversing analgesia. Gastrointestinal transit time (lactulose hydrogen breath test) was measured in 14 volunteers with oral and intravenous placebo, oral placebo and intravenous morphine (0.05 mg x kg(-1)), and oral ADL 8-2698 (4 mg) and intravenous morphine (0.05 mg x kg(-1)) in a double blind, cross-over study. Morphine prolonged gastrointestinal transit time from 69 to 103 minutes (P = .005); this was prevented by ADL 8-2698 (P = .004). Postoperatively, 45 patients were randomly assigned in a double-blind fashion to receive ADL 8-2698 (4 mg) or placebo and intravenous morphine (0.15 mg/kg) or to receive oral and intravenous placebo. Analgesia and pupil constriction were measured. Morphine analgesia and pupil constriction were unaffected by ADL 8-2698 and differed from placebo (P < .002). We conclude that ADL 8-2698 prevents morphine-induced increases in gastrointestinal transit time by means of selective peripheral opioid anitagonism without affecting central opioid analgesia.
机译:ADL-8-2698是一种新型的外周限制性阿片拮抗剂,可选择性预防阿片类药物引起的胃肠道作用而不逆转镇痛作用。测量了14名志愿者的胃肠道运输时间(乳酸氢呼吸试验),包括口服和静脉安慰剂,口服安慰剂和静脉吗啡(0.05 mg x kg(-1)),口服ADL 8-2698(4 mg)和静脉吗啡( 0.05 mg x kg(-1))进行双盲交叉研究。吗啡将胃肠道的传输时间从69分钟延长至103分钟(P = 0.005); ADL 8-2698(P = .004)防止了这种情况。术后,以双盲方式随机分配了45名患者,分别接受ADL 8-2698(4 mg)或安慰剂和静脉吗啡(0.15 mg / kg)或口服和静脉安慰剂。测量镇痛和瞳孔收缩。吗啡镇痛和瞳孔狭窄不受ADL 8-2698的影响,与安慰剂有所不同(P <.002)。我们得出的结论是,ADL 8-2698通过选择性外周阿片类药物拮抗作用防止吗啡诱导的胃肠道转运时间增加,而不会影响中枢阿片类药物的镇痛作用。

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