一种新的白三烯合成选择性抑制剂BAY X1005:药理学和药代动力学。

Journal of lipid mediators Pub Date : 1993-03-01
R Müller-Peddinghaus, R Fruchtmann, H J Ahr, B Beckermann, K Bühner, B Fugmann, B Junge, M Matzke, C Kohlsdorfer, S Raddatz
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引用次数: 0

摘要

对映体BAY X1005 [(R)-2-[4-(喹啉-2-酰基甲氧基)苯基]-2-环戊基乙酸]能有效抑制不同物种PMNL中LTB4的合成(IC50 μ mol/l,人0.22,大鼠0.026,小鼠0.039)和小鼠巨噬细胞中LTC4的合成(IC50 0.021 μ mol/l)。由于高蛋白结合,体外抑制全血LTB4合成的效价经RIA测定降至17 μ mol/l。BAY X1005对5-脂氧合酶途径具有选择性,使12-HETE和HHT保持不变,在人全血中测定。口服后,在花生四烯酯诱导的小鼠耳部炎症试验中,BAY X1005抑制水肿形成和髓过氧化物酶活性(ED50分别为48.7和7.9)。在全血中发现大鼠离体口服LTB4合成抑制活性(ED50为11.8 mg/kg)。BAY X1005具有很高的生物利用度(86%),Cmax为13 mg/l,在10 mg/kg p.o的大鼠体内可达3.5 h的1/2。因此,白三烯合成抑制剂BAY X1005的药效学、药代动力学特征和安全性方面允许在人体中测试其治疗炎症和过敏性疾病的潜力。
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BAY X1005, a new selective inhibitor of leukotriene synthesis: pharmacology and pharmacokinetics.

The enantiomer BAY X1005 [(R)-2-[4-(quinolin-2-yl-methoxy)phenyl]-2-cyclopentyl acetic acid] potently inhibits LTB4 synthesis in isolated PMNL of various species (IC50 mumol/l, human 0.22, rat 0.026, mouse 0.039) and LTC4 synthesis in mouse macrophages (IC50 0.021 mumol/l). Due to high protein binding the in vitro potency for LTB4 synthesis inhibition in whole blood is lowered to 17 mumol/l as determined by RIA. BAY X1005 is selective for the 5-lipoxygenase pathway leaving 12-HETE and HHT unaltered, as determined in human whole blood. After oral application BAY X1005 inhibits edema formation and myeloperoxidase activity in the arachidonate-induced mouse ear inflammation test (ED50 48.7 and 7.9, respectively). Oral activity in the rat ex vivo is found in whole blood for LTB4 synthesis inhibition (ED50 11.8 mg/kg p.o.). BAY X1005 demonstrates a high bioavailability (f 86%) with a Cmax of 13 mg/l and t1/2 of 3.5 h in the rat at 10 mg/kg p.o. Thus, the pharmacodynamic, pharmacokinetic profile and safety aspects of the leukotriene synthesis inhibitor BAY X1005 allow testing in man for its therapeutic potential in inflammatory and allergic diseases.

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