SELECTIVE-INHIBITION OF CYCLOOXYGENASE-2

被引：141

作者：

KLEIN, T

NUSING, RM

PFEILSCHIFTER, J

ULLRICH, V

机构：

[1] UNIV KONSTANZ,FAC BIOL,D-78434 CONSTANCE,GERMANY

[2] UNIV BASEL,BIOCTR,DEPT PHARMACOL,CH-4056 BASEL,SWITZERLAND

来源：

BIOCHEMICAL PHARMACOLOGY | 1994年 / 48卷 / 08期

关键词：

NONSTEROIDAL ANTIINFLAMMATORY DRUGS; CYCLOOXYGENASE; ARACHIDONIC ACID METABOLISM; INTERLEUKIN; 1; MESANGIAL CELL; REVERSE TRANSCRIPTION POLYMERASE CHAIN REACTION;

D O I：

10.1016/0006-2952(94)90205-4

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Cyclooxygenase (COX), a key enzyme in the formation of prostanoids, is known to exist in two isoforms: an inducible enzyme (COX 2,) and a constitutive form (COX 1). Both enzymes are inhibited by non-steroidal anti-inflammatory drugs (NSAID), but only marginal selectivity has thus far been reported. In this study, we report on a novel selective inhibitor of COX 2, CGP 28238 (6-(2,4-difluorophenoxy)-5-methyl-sulfonylamino-1-indanone). Human washed platelets were used as a source of COX 1. For IL-1 stimulated rat mesangial cells we demonstrated the almost exclusive presence of COX 2 in western blot and mRNA analysis. Therefore these two model systems were chosen for selectivity testing. With an IC50 value of 15 nM, CGP 28238 blocked COX 2 activity in a similar concentration range to that of other potent NSAID such as indomethacin and diclofenac (IC50 = 1.17-8.9 nM). However, in contrast to these reference NSAIDs, CGP 28238 was at least 1000-fold less potent in inhibiting COX 1. Using other cell systems reported to express COX 1 or COX 2, we obtained a similar selectivity for COX 2. Thus, on the basis of our findings, CGP 28238 is a novel, highly potent and selective inhibitor of COX 2 and may be a lead compound for a new generation of potent anti-inflammatory drugs with an improved side-effect profile.

引用

页码：1605 / 1610

页数：6

共 22 条

[1]

DEWITT DL, 1993, AM J MED, V95, pA2

[2] NS-398, A NEW ANTIINFLAMMATORY AGENT, SELECTIVELY INHIBITS PROSTAGLANDIN-G/H SYNTHASE CYCLOOXYGENASE (COX-2) ACTIVITY IN-VITRO [J].

FUTAKI, N ;

TAKAHASHI, S ;

YOKOYAMA, M ;

ARAI, I ;

HIGUCHI, S ;

OTOMO, S .

PROSTAGLANDINS, 1994, 47 (01) :55-59

[3]

HECKER M, 1989, J BIOL CHEM, V264, P141

[4]

HERSCHMAN HR, 1993, J LIPID MEDIATOR, V6, P89

[5] INDUCTION OF THROMBOXANE SYNTHASE AND PROSTAGLANDIN ENDOPEROXIDE SYNTHASE MESSENGER-RNAS IN HUMAN ERYTHROLEUKEMIA-CELLS BY PHORBOL ESTER [J].

IHARA, H ;

YOKOYAMA, C ;

MIYATA, A ;

KOSAKA, T ;

NUSING, R ;

ULLRICH, V ;

TANABE, T .

FEBS LETTERS, 1992, 306 (2-3) :161-164

[6] INTERLEUKIN-1-INDUCED CYCLOOXYGENASE-2 EXPRESSION IS SUPPRESSED BY CYCLOSPORINE-A IN RAT MESANGIAL CELLS [J].

MARTIN, M ;

NEUMANN, D ;

HOFF, T ;

RESCH, K ;

DEWITT, DL ;

GOPPELTSTRUEBE, M .

KIDNEY INTERNATIONAL, 1994, 45 (01) :150-158

[7]

MATSUNAGA H, 1972, ANN CHIM ACTA, V58, P228

[8]

MEADE EA, 1993, J LIPID MEDIATOR, V6, P119

[9]

MEADE EA, 1993, J BIOL CHEM, V268, P6610

[10] PHYSIOLOGY OF THE MESANGIAL CELL [J].

MENE, P ;

SIMONSON, MS ;

DUNN, MJ .

PHYSIOLOGICAL REVIEWS, 1989, 69 (04) :1347-1424

← 1 2 3 →