Landoni M F, Lees P
Department of Veterinary Basic Sciences, Royal Veterinary College, Hatfield, Herts, UK.
Equine Vet J. 1995 Jul;27(4):247-56. doi: 10.1111/j.2042-3306.1995.tb03073.x.
A comparative study in horses of the pharmacokinetics (PK) and pharmacodynamics (PD) of 2 extensively used nonsteroidal anti-inflammatory drugs (NSAIDs), flunixin (FXN) and ketoprofen (KTP), was carried out applying PK/PD modelling. To evaluate the anti-inflammatory properties of these drugs a model of acute inflammation, comprising surgically implanted subcutaneous tissue cages stimulated by intracaveal injection of carrageenan, was used. FXN elimination half-life (T1/2 beta) in plasma was 3.37 +/- 1.09 h. However, in exudate a much longer T1/2 beta was obtained (15.99 +/- 3.80 h). Apparent volume of distribution (Vdarea) for FXN was 0.317 +/- 0.126 l/kg and body clearance (ClB) was 0.058 +/- 0.004 l/kg/h. KTP displayed enantioselective pharmacokinetics, the S(+) enantiomer being predominant in plasma, exudate and transudate. T1/2 beta values for R(-) and S(+)KTP were, respectively, 1.09 +/- 0.19 h and 1.51 +/- 0.45 h (plasma) and 19.73 +/- 2.72 h and 22.64 +/- 4.34 h (exudate), respectively. R(-)KTP was cleared more rapidly than the S(+) enantiomer. ClB values were 0.277 +/- 0.035 l/kg/h and 0.202 +/- 0.022 l/kg/h, respectively. FXN and KTP pharmacodynamics was evaluated by determining their inhibitory effects on serum thromboxane (Tx)B2, exudate prostaglandin (PG)E2, leukotriene (LT)B4 and beta-glucuronidase (beta-glu) and intradermal bradykinin-induced swelling. Both drugs produced marked inhibition of serum TxB2 synthesis for up to 24 h, with no significant differences between the drugs. FXN was a more potent inhibitor of exudate PGE2, the EC50 for FXN being lower (P < 0.01) than that for KTP (0.019 +/- 0.010 microgram/ml and 0.057 +/- 0.009 microgram/ml, respectively). Neither drug had any effect on exudate LTB4 concentration. Differences between the 2 drugs were observed for the inhibition of beta-glu, the Emax for KTP being higher (P < 0.01) than for FXN. However, no differences were observed in other PD parameters. Both FXN and KTP inhibited bradykinin-induced swelling. Differences between the drugs were obtained for Emax, which was greater for FXN (P < 0.01) than for KTP. Equilibration half-life (T1/2Ke0) also differed, being much longer (P < 0.01) for FXN than for KTP. PK/PD modelling proved to be a useful and novel analytical technique for studying the pharmacodynamics of NSAIDs, with the advantage over classical in vitro methods that it provides data in the whole animal. By quantifying action-concentration interrelationships through PK-PD modelling, it is possible to shed light on molecular mechanisms of drug action, and establish probable differences in mechanisms of action between structurally similar drugs.(ABSTRACT TRUNCATED AT 400 WORDS)
运用药代动力学/药效学(PK/PD)模型,对两种广泛使用的非甾体抗炎药(NSAIDs)氟尼辛(FXN)和酮洛芬(KTP)在马匹中的药代动力学(PK)和药效学(PD)进行了比较研究。为评估这些药物的抗炎特性,使用了一种急性炎症模型,该模型包括通过向皮下植入的组织笼腔内注射角叉菜胶来刺激的手术植入皮下组织笼。FXN在血浆中的消除半衰期(T1/2β)为3.37±1.09小时。然而,在渗出液中获得了长得多的T1/2β(15.99±3.80小时)。FXN的表观分布容积(Vdarea)为0.317±0.126升/千克,机体清除率(ClB)为0.058±0.004升/千克/小时。KTP表现出对映体选择性药代动力学,S(+)对映体在血浆、渗出液和漏出液中占主导。R(-)和S(+)KTP的T1/2β值分别为1.09±0.19小时和1.51±0.45小时(血浆)以及19.73±2.72小时和22.64±4.34小时(渗出液)。R(-)KTP的清除速度比S(+)对映体更快。ClB值分别为0.277±0.035升/千克/小时和0.202±0.022升/千克/小时。通过测定FXN和KTP对血清血栓素(Tx)B2、渗出液前列腺素(PG)E2、白三烯(LT)B4和β-葡萄糖醛酸酶(β-glu)的抑制作用以及皮内缓激肽诱导的肿胀,评估了它们的药效学。两种药物均对血清TxB2合成产生显著抑制,持续长达24小时,两种药物之间无显著差异。FXN是渗出液PGE2更有效的抑制剂,FXN的半数有效浓度(EC50)低于KTP(分别为0.019±0.010微克/毫升和0.057±0.009微克/毫升,P<0.01)。两种药物对渗出液LTB4浓度均无影响。在对β-glu的抑制方面观察到两种药物之间存在差异,KTP的最大效应(Emax)高于FXN(P<0.01)。然而,在其他PD参数方面未观察到差异。FXN和KTP均抑制缓激肽诱导的肿胀。在Emax方面获得了两种药物之间的差异,FXN的Emax大于KTP(P<0.01)。平衡半衰期(T1/2Ke0)也不同,FXN比KTP长得多(P<0.01)。PK/PD模型被证明是研究NSAIDs药效学的一种有用且新颖的分析技术,与传统体外方法相比具有优势,即它能在完整动物中提供数据。通过PK-PD模型量化作用-浓度相互关系,有可能阐明药物作用的分子机制,并确定结构相似药物之间作用机制的可能差异。(摘要截断于400字)
Zotero 插件