ICI D2138的临床前药理学，一种强效口服活性5-脂氧合酶非氧化还原抑制剂。

Pre-clinical pharmacology of ICI D2138, a potent orally-active non-redox inhibitor of 5-lipoxygenase.

作者信息

McMillan R M, Spruce K E, Crawley G C, Walker E R, Foster S J

机构信息

ICI Pharmaceuticals, Alderley Park, Macclesfield, Cheshire.

出版信息

Br J Pharmacol. 1992 Dec;107(4):1042-7. doi: 10.1111/j.1476-5381.1992.tb13404.x.

DOI:10.1111/j.1476-5381.1992.tb13404.x

PMID:1334748

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1907929/

Abstract

This paper describes the pre-clinical pharmacology of ICI D2138, a potent orally-active non-redox inhibitor of 5-lipoxygenase which is undergoing clinical evaluation. 2. ICI D2138 potently inhibited leukotriene synthesis in murine peritoneal macrophages (IC50 = 3 nM) and human blood (IC50 = 20 nM). In human and dog blood, ICI D2138 did not inhibit thromboxane B2 synthesis at a concentration of 500 microM, thus the selectivity ratio (cyclo-oxygenase: 5-lipoxygenase) was greater than 20,000. In contrast, zileuton (a 5-lipoxygenase inhibitor also undergoing clinical evaluation) exhibited a selectivity ratio of 15-100. 3. ICI D2138 potently and dose-dependently inhibited ex vivo leukotriene B4 (LTB4) synthesis by rat blood with ED50 values of 0.9, 4.0 and 80.0 mg kg-1 p.o. at 3, 10 and 20 h respectively after dosing. Similar activity was observed for inhibition of LTB4 production in a zymosan-inflamed rat air pouch model. Zileuton produced ED50 values of 5 and 20 mg kg-1 at 3 and 10 h respectively. 4. Oral administration of 1, 3 or 10 mg kg-1 ICI D2138 to dogs produced maximal inhibition of ex vivo LTB4 synthesis by blood for 5, 9 and 31 h respectively. A dose of 5 mg kg-1 p.o. of zileuton caused maximal inhibition of LTB4 for 24 h. 5. Oral administration of 10 mg kg-1 ICI D2138 caused total inhibition of LTB4 production in zymosan-inflamed rabbit knee joint. 6. Topical administration of ICI D2138 to rabbit skin caused a dose-related inhibition of arachidonic acid-induced plasma extravasation with an ID30 of 1.08 nmol per site. Zileuton was approximately 40 times less potent.7. Oral anti-inflammatory activity was assessed in an arachidonic acid-induced mouse ear oedema model in animals treated with indomethacin to block pro-inflammatory prostanoids. ICI D2138, given orally, caused dose-dependent inhibition of oedema with an approximate ID50 of 1.8 mg kg'. Zileuton was approximately 10 times less potent.8. ICI D2138 caused a dose-dependent inhibition of antigen-induced broncho-constriction in guineapigs with an approximate ID50 of 0.1 mg kg-', i.v. Zileuton was approximately 10 times less potent.9. In view of the pharmacological profile described here, ICI D2138 has the potential to provide improved clinical efficacy compared to existing lipoxygenase inhibitors such as zileuton.

摘要

本文描述了ICI D2138的临床前药理学特性，它是一种正在进行临床评估的强效口服活性5-脂氧合酶非氧化还原抑制剂。2. ICI D2138能有效抑制小鼠腹腔巨噬细胞（IC50 = 3 nM）和人血液（IC50 = 20 nM）中的白三烯合成。在人和犬的血液中，500 microM浓度的ICI D2138不抑制血栓素B2的合成，因此其选择性比率（环氧化酶：5-脂氧合酶）大于20,000。相比之下，齐留通（一种也在进行临床评估的5-脂氧合酶抑制剂）的选择性比率为15 - 100。3. ICI D2138能有效且剂量依赖性地抑制大鼠血液离体白三烯B4（LTB4）的合成，给药后3、10和20小时的口服ED50值分别为0.9、4.0和80.0 mg kg-1。在酵母聚糖诱发炎症的大鼠气囊模型中，观察到对LTB4产生的类似抑制活性。齐留通在3和10小时的ED50值分别为5和20 mg kg-1。4. 给犬口服1、3或10 mg kg-1的ICI D2138，分别对血液离体LTB4合成产生5、9和31小时的最大抑制。口服5 mg kg-1的齐留通对LTB4产生24小时的最大抑制。5. 给酵母聚糖诱发炎症的兔膝关节口服10 mg kg-1的ICI D2138可完全抑制LTB4的产生。6. 给兔皮肤局部应用ICI D2138可剂量依赖性地抑制花生四烯酸诱导的血浆外渗，每个部位的ID30为1.08 nmol。齐留通的效力约低40倍。7. 在给予吲哚美辛以阻断促炎前列腺素的动物中，通过花生四烯酸诱导的小鼠耳水肿模型评估口服抗炎活性。口服ICI D2138可剂量依赖性地抑制水肿，近似ID50为约1.8 mg kg-1。齐留通的效力约低10倍。8. ICI D2138静脉注射可剂量依赖性地抑制豚鼠抗原诱导的支气管收缩，近似ID50为0.1 mg kg-1。齐留通的效力约低10倍。9. 鉴于此处描述的药理学特性，与现有的脂氧合酶抑制剂如齐留通相比，ICI D2138有潜力提供更好的临床疗效。