Haubrich D R, Ward S J, Baizman E, Bell M R, Bradford J, Ferrari R, Miller M, Perrone M, Pierson A K, Saelens J K
Department of Pharmacology, Sterling Drug Inc., Sterling Research Group, Rensselaer, New York.
J Pharmacol Exp Ther. 1990 Nov;255(2):511-22.
Pravadoline is a new chemical entity with analgesic activity in humans. This report describes the pharmacology of pravadoline and compares the activity of pravadoline with that of two major classes of analgesics, the opioids and the nonsteroidal anti-inflammatory drugs (NSAIDs). Like the NSAIDs, pravadoline inhibited the synthesis of prostaglandins (PGs) in mouse brain both in vitro (IC50, 4.9 microM) and ex vivo (ED50, 20 mg/kg p.o.) and displayed antinociceptive activity in rodents subjected to a variety of chemical, thermal and mechanical nociceptive stimuli. Administration of pravadoline prevented the writhing response induced by i.p. administration of acetylcholine (ED50, 41 mg/kg p.o.) or PGE2 (ED50, 24 mg/kg p.o.) and prolonged the response latency induced by tail immersion in hot water at a temperature of 55 degrees C (minimum effective dose, 100 mg/kg s.c.). In the rat, treatment with pravadoline prevented acetic acid-induced writhing (ED50, 15 mg/kg p.o.), brewer's yeast-induced hyperalgesia (Randall-Selitto test) (minimum effective dose, 1 mg/kg p.o.), the nociceptive response induced by paw flexion in the adjuvant-arthritic rat (ED50, 41 mg/kg p.o.) and bradykinin-induced head and forepaw flexion (ED50, 78 mg/kg, p.o.). The antinociceptive activity of pravadoline cannot be explained by an opioid mechanism, because pravadoline-induced antinociception was not antagonized by naloxone (1 mg/kg s.c.) and pravadoline did not bind to opioid receptors at concentrations up to 10 microM. However, like the opioid analgesics, pravadoline diminished the electrically induced twitch response of mouse vas deferens preparations, but, in contrast to opioids, this action of pravadoline was not attenuated by naloxone. The possibility is discussed that this effect of pravadoline upon isolated tissues may contribute to its antinociceptive activity. In contrast to NSAIDs, pravadoline was more potent ex vivo as an inhibitor of the formation of PGs in brain vs. stomach. In addition, pravadoline failed to produce gastrointestinal lesions when administered p.o. to rats or mice, and did not possess significant anti-inflammatory activity at antinociceptive doses. Also unlike NSAIDs, pravadoline inhibited rat gastrointestinal transit when administered at doses similar to those which were antinociceptive. The overall pharmacologic profile of pravadoline suggests that the compound may be capable of managing more diverse or more severe pain than is achieved by anti-inflammatory analgesics, without producing side effects commonly associated with either the opioid or the nonopioid analgesics.
普拉瓦多林是一种对人体具有镇痛活性的新型化学实体。本报告描述了普拉瓦多林的药理学特性,并将其活性与两类主要镇痛药(阿片类药物和非甾体抗炎药(NSAIDs))进行了比较。与NSAIDs一样,普拉瓦多林在体外(IC50,4.9 microM)和体内(ED50,20 mg/kg口服)均能抑制小鼠脑中前列腺素(PGs)的合成,并在受到各种化学、热和机械性伤害性刺激的啮齿动物中表现出抗伤害感受活性。给予普拉瓦多林可预防腹腔注射乙酰胆碱(ED50,41 mg/kg口服)或PGE2(ED50,24 mg/kg口服)诱导的扭体反应,并延长在55摄氏度热水中尾浸诱导的反应潜伏期(最小有效剂量,100 mg/kg皮下注射)。在大鼠中,用普拉瓦多林治疗可预防乙酸诱导的扭体反应(ED50,15 mg/kg口服)、啤酒酵母诱导的痛觉过敏(Randall-Selitto试验)(最小有效剂量,1 mg/kg口服)、佐剂性关节炎大鼠中爪屈曲诱导的伤害性反应(ED50,41 mg/kg口服)以及缓激肽诱导的头部和前爪屈曲(ED50,78 mg/kg,口服)。普拉瓦多林的抗伤害感受活性不能用阿片类机制来解释,因为纳洛酮(1 mg/kg皮下注射)不能拮抗普拉瓦多林诱导的抗伤害感受作用,且普拉瓦多林在浓度高达10 microM时不与阿片受体结合。然而,与阿片类镇痛药一样,普拉瓦多林可减弱小鼠输精管制剂的电诱导抽搐反应,但与阿片类药物不同的是,普拉瓦多林的这一作用不会被纳洛酮减弱。讨论了普拉瓦多林对离体组织的这种作用可能有助于其抗伤害感受活性的可能性。与NSAIDs不同,普拉瓦多林在体内作为脑内PGs形成抑制剂比在胃中更有效。此外,普拉瓦多林口服给药于大鼠或小鼠时不会产生胃肠道损伤,且在抗伤害感受剂量下不具有显著的抗炎活性。同样与NSAIDs不同的是,普拉瓦多林在以与抗伤害感受剂量相似的剂量给药时会抑制大鼠胃肠道蠕动。普拉瓦多林的总体药理学特征表明,该化合物可能能够处理比抗炎镇痛药更广泛或更严重的疼痛,而不会产生通常与阿片类或非阿片类镇痛药相关的副作用。
