A human whole blood assay for clinical evaluation of biochemical efficacy of cyclooxygenase inhibitors

被引：267

作者：

Brideau, C

Kargman, S

Liu, S

Dallob, AL

Ehrich, EW

Rodger, IW

Chan, CC

机构：

[1] MERCK FROSST CTR THERAPEUT RES, DEPT PHARMACOL, POINTE CLAIRE, PQ H9R 4P8, CANADA

[2] MERCK FROSST CTR THERAPEUT RES, DEPT BIOCHEM, POINTE CLAIRE, PQ H9R 4P8, CANADA

[3] MERCK FROSST CTR THERAPEUT RES, DEPT MOLEC PHARMACOL, POINTE CLAIRE, PQ H9R 4P8, CANADA

[4] MERCK & CO INC, DEPT CLIN PHARMACOL, RAHWAY, NJ 07065 USA

来源：

INFLAMMATION RESEARCH | 1996年 / 45卷 / 02期

关键词：

Cox-2; inhibitors; CGP-28238; NS-398; SC-58125; L-745,337;

D O I：

10.1007/BF02265118

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

In this study, PGE(2) levels in lipopolysaccharide (LPS)-challenged human whole blood and TxB(2) levels following blood coagulation were measured as biochemical index for cyclooxygenase (Cox)-2 and Cox-1 activity respectively. Incubation of human mononuclear cells isolated from whole blood with LPS (100 mu g/mL) induced a time-dependent increase in the expression of Cox-2 protein (>100 fold at 24hr). This is associated with increases in PGE(2) production and free arachidonate release in the plasma. Cox-1 protein was detected in the human mononuclear cells at time zero but was not induced by either LPS or PBS. Most non-steroidal antiinflammatory drugs (NSAIDs) are more potent at inhibiting Cox-1 than Cox-2. Five experimental compounds CGP-28238, Dup-697, NS-398, SC-58125 and L-745,337, have a greater selectivity for Cox-2. Indomethacin at a single oral dose (25 mg) inhibited approximately 90% the whole blood Cox-2 and Cox-1 activities ex vivo in healthy subjects. These results support the use of this assay to assess the biochemical efficacy of selective Cox-2 inhibitors in clinical trials.

引用

页码：68 / 74

页数：7

共 38 条

[11] KARGMAN SL, 1995, CANCER RES, V55, P2556
[12] NONSTEROIDAL ANTIINFLAMMATORY DRUG-USE IN RELATION TO MAJOR UPPER GASTROINTESTINAL-BLEEDING
KAUFMAN, DW
KELLY, JP
SHEEHAN, JE
LASZLO, A
WIHOLM, BE
ALFREDSSON, L
KOFF, RS
SHAPIRO, S
[J]. CLINICAL PHARMACOLOGY & THERAPEUTICS, 1993, 53 (04) : 485 - 494
[13] CLONING AND EXPRESSION OF RAT PROSTAGLANDIN ENDOPEROXIDE SYNTHASE (CYCLOOXYGENASE)-2 CDNA
KENNEDY, BP
CHAN, CC
CULP, SA
CROMLISH, WA
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1993, 197 (02) : 494 - 500
[14] KUJUBU DA, 1991, J BIOL CHEM, V266, P12866
[15] CLEAVAGE OF STRUCTURAL PROTEINS DURING ASSEMBLY OF HEAD OF BACTERIOPHAGE-T4
LAEMMLI, UK
[J]. NATURE, 1970, 227 (5259) : 680 - +
[16] RISKS OF BLEEDING PEPTIC-ULCER ASSOCIATED WITH INDIVIDUAL NONSTEROIDAL ANTIINFLAMMATORY DRUGS
LANGMAN, MJS
WEIL, J
WAINWRIGHT, P
LAWSON, DH
RAWLINS, MD
LOGAN, RFA
MURPHY, M
VESSEY, MP
COLINJONES, DG
[J]. LANCET, 1994, 343 (8905) : 1075 - 1078
[17] LEE SH, 1992, J BIOL CHEM, V267, P25934
[18] LIPOPOLYSACCHARIDE BINDING-PROTEIN ENHANCES THE RESPONSIVENESS OF ALVEOLAR MACROPHAGES TO BACTERIAL LIPOPOLYSACCHARIDE - IMPLICATIONS FOR CYTOKINE PRODUCTION IN NORMAL AND INJURED LUNGS
MARTIN, TR
MATHISON, JC
TOBIAS, PS
LETURCQ, DJ
MORIARTY, AM
MAUNDER, RJ
ULEVITCH, RJ
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1992, 90 (06) : 2209 - 2219
[19] SELECTIVE-INHIBITION OF INDUCIBLE CYCLOOXYGENASE-2 IN-VIVO IS ANTIINFLAMMATORY AND NONULCEROGENIC
MASFERRER, JL
ZWEIFEL, BS
MANNING, PT
HAUSER, SD
LEAHY, KM
SMITH, WG
ISAKSON, PC
SEIBERT, K
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (08) : 3228 - 3232
[20] MEADE EA, 1993, J BIOL CHEM, V268, P6610

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