STEREOSELECTIVE CYCLOOXYGENASE INHIBITION IN CELLULAR-MODELS BY THE ENANTIOMERS OF KETOPROFEN

被引：71

作者：

SUESA, N ^{[1
]}

FERNANDEZ, MF ^{[1
]}

GUTIERREZ, M ^{[1
]}

RUFAT, MJ ^{[1
]}

ROTLLAN, E ^{[1
]}

CALVO, L ^{[1
]}

MAULEON, D ^{[1
]}

CARGANICO, G ^{[1
]}

机构：

[1] LABS MENARINI SA,DEPT RES & DEV,ALFONSO XII 587,E-08912 BADALONA,SPAIN

来源：

CHIRALITY | 1993年 / 5卷 / 08期

关键词：

NSAIDS; ENANTIOSELECTIVITY; PROSTAGLANDIN E2; THROMBOXANE B2; HUVEC; PMN; KERATINOCYTES; P388D1; PLATELETS;

D O I：

10.1002/chir.530050805

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

The pharmacological activity of rac-ketoprofen and its enantiomers was investigated in vitro using different cellular models. The effect of these compounds on arachidonic acid metabolism was assessed by measuring the inhibition of prostanoid generation under the action of several agonists. Thus, we have evaluated the inhibition of (1) thromboxane B2 synthesis in rabbit platelets and human polymorphonuclear leukocytes (PMNs), (2) prostaglandin E2 Synthesis in three cultured cells, namely human umbilical vein endothelial cells (HUVEC), human keratinocytes, and mouse macrophage-like P388D1 cells. The IC50 values found for (+)-(S)-ketoprofen were in the range between 0.1 nM and 0.8 muM, being slightly lower in all models than those found for rac-ketoprofen (0. 4 nM-3 muM). On the other hand, (-)-(R)-ketoprofen showed inhibition of cyclooxygenase only at concentrations two or three orders of magnitude higher than those required for the (+)-(S) enantiomer. These results, obtained with cell types of relevance for inflammatory processes and with compounds of high optical purity, demonstrate that the prostanoid biosynthesis inhibition caused by the drug rac-ketoprofen is exclusively due to its dextrorotatory enantiomer. (C) 1993 Wiley-Liss, Inc.

引用

页码：589 / 595

页数：7

共 34 条

[1] PHARMACOLOGICAL DIFFERENCES BETWEEN OPTICAL ISOMERS OF IBUPROFEN - EVIDENCE FOR METABOLIC INVERSION OF (-)-ISOMER [J].

ADAMS, SS ;

BRESLOFF, P ;

MASON, CG .

JOURNAL OF PHARMACY AND PHARMACOLOGY, 1976, 28 (03) :256-257

[2] KERATINOCYTES AS INITIATORS OF INFLAMMATION [J].

BARKER, JNWN ;

MITRA, RS ;

GRIFFITHS, CEM ;

DIXIT, VM ;

NICKOLOFF, BJ .

LANCET, 1991, 337 (8735) :211-214

[3] MODELS FOR EVALUATING THE ANTI-INFLAMMATORY EFFECTS OF INHIBITORS OF ARACHIDONIC-ACID METABOLISM [J].

BLACKHAM, A ;

NORRIS, AA ;

WOODS, FAM .

JOURNAL OF PHARMACY AND PHARMACOLOGY, 1985, 37 (11) :787-793

[4] INHIBITION BY ANTI-INFLAMMATORY DRUGS OF PROSTAGLANDIN PRODUCTION IN CULTURED MACROPHAGES - FACTORS INFLUENCING THE APPARENT DRUG EFFECTS [J].

BRUNE, K ;

RAINSFORD, KD ;

WAGNER, K ;

PESKAR, BA .

NAUNYN-SCHMIEDEBERGS ARCHIVES OF PHARMACOLOGY, 1981, 315 (03) :269-&

[5] NON-STEROID ANTI-INFLAMMATORY DRUGS - INFLUENCE OF EXTRA-CELLULAR PH ON BIODISTRIBUTION AND PHARMACOLOGICAL EFFECTS [J].

BRUNE, K ;

GRAF, P .

BIOCHEMICAL PHARMACOLOGY, 1978, 27 (04) :525-530

[6]

BRUNE K, 1985, AGENTS ACTIONS, V17, P342

[7]

BUCHANAN MR, 1988, HAEMOSTASIS, V18, P360

[8] BIOLOGICAL-ACTIVITY OF INDOPROFEN AND ITS OPTICAL ISOMERS [J].

BUTTINONI, A ;

FERRARI, M ;

COLOMBO, M ;

CESERANI, R .

JOURNAL OF PHARMACY AND PHARMACOLOGY, 1983, 35 (09) :603-604

[9] THE METABOLIC CHIRAL INVERSION AND DISPOSITIONAL ENANTIOSELECTIVITY OF THE 2-ARYLPROPIONIC ACIDS AND THEIR BIOLOGICAL CONSEQUENCES [J].

CALDWELL, J ;

HUTT, AJ ;

FOURNELGIGLEUX, S .

BIOCHEMICAL PHARMACOLOGY, 1988, 37 (01) :105-114

[10] THE (+)-ENANTIOMER IS RESPONSIBLE FOR THE ANTIPLATELET AND ANTIINFLAMMATORY ACTIVITY OF (+/-)-INDOBUFEN [J].

CERLETTI, C ;

MANARINI, S ;

COLOMBO, M ;

TAVANI, A .

JOURNAL OF PHARMACY AND PHARMACOLOGY, 1990, 42 (12) :885-887

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