ORAL LEUKOTRIENE INHIBITOR (MK-886) BLOCKS ALLERGEN-INDUCED AIRWAY RESPONSES

被引：141

作者：

FRIEDMAN, BS ^{[1
]}

BEL, EH ^{[1
]}

BUNTINX, A ^{[1
]}

TANAKA, W ^{[1
]}

HAN, YHR ^{[1
]}

SHINGO, S ^{[1
]}

SPECTOR, R ^{[1
]}

STERK, P ^{[1
]}

机构：

[1] LEIDEN UNIV HOSP,2333 AA LEIDEN,NETHERLANDS

来源：

AMERICAN REVIEW OF RESPIRATORY DISEASE | 1993年 / 147卷 / 04期

关键词：

D O I：

10.1164/ajrccm/147.4.839

中图分类号：

R56 [呼吸系及胸部疾病];

学科分类号：

摘要：

To elucidate the role of leukotrienes (LT) in allergic asthma in humans the effect of MK-886, an LT biosynthesis inhibitor, was evaluated on antigen-induced early (EAR) and late (LAR) asthmatic reactions and bronchial responsiveness to histamine. Eight atopic men participated in a two-part, double-blind, placebo-controlled, crossover trial. MK-886 was administered in two oral doses of 500 mg and 250 mg, 1 h before and 2 h after allergen inhalation, respectively. Biochemical effects of MK-886 were evaluated by the inhibition of urinary LTE4 excretion and calcium ionophore-stimulated LTB4 biosynthesis in whole blood ex vivo. MK-886 significantly inhibited the EAR by 58.4% (AUC0-3 h) and the LAR by 43.6% (AUC3-7 h) when compared with placebo (p < 0.01). There was no difference in PC20 histamine 30 h post allergen challenge between MK-886 and placebo (0.33 and 0.27 doubling doses, p > 0.1). MK-886 inhibited calcium ionophore-stimulated LTB4 production in whole blood (54.2 +/- 25.6%) for up to 6 h post allergen challenge. LTE4 excretion in urine was inhibited by 51.5% during the EAR by as much as 80% during the LAR. This indicates that LT play a role in allergen-induced asthmatic reactions in humans in vivo and that LT synthesis inhibitors such as MK-886 should be further explored for the treatment of asthma.

引用

页码：839 / 844

页数：6

共 33 条

[1] THE EFFECT OF AN INHALED LEUKOTRIENE ANTAGONIST, L-648,051, ON EARLY AND LATE ASTHMATIC REACTIONS AND SUBSEQUENT INCREASE IN AIRWAY RESPONSIVENESS IN MAN
BEL, EH
TIMMERS, MC
DIJKMAN, JH
STAHL, EG
STERK, PJ
[J]. JOURNAL OF ALLERGY AND CLINICAL IMMUNOLOGY, 1990, 85 (06) : 1067 - 1075
[2] LEUKOTRIENE-B4 INCREASES PULMONARY TRANSVASCULAR FILTRATION BY A NEUTROPHIL-INDEPENDENT MECHANISM
BURGESS, CA
MCCANDLESS, BK
COOPER, JA
MALIK, AB
[J]. JOURNAL OF APPLIED PHYSIOLOGY, 1990, 68 (03) : 1260 - 1264
[3] RADIOIMMUNOASSAY OF LTB4 AND 6-TRANS LTB4 - ANALYTICAL AND PHARMACOLOGICAL CHARACTERIZATION OF IMMUNOREACTIVE LTB4 IN IONOPHORE STIMULATED HUMAN-BLOOD
CAREY, F
FORDER, RA
[J]. PROSTAGLANDINS LEUKOTRIENES AND MEDICINE, 1986, 22 (01): : 57 - 70
[4] COCKCROFT DW, 1987, AM REV RESPIR DIS, V135, P264
[5] COCKCROFT DW, 1987, ANN ALLERGY, V59, P89
[6] ALLERGEN CHALLENGE OF LUNG-TISSUE FROM ASTHMATICS ELICITS BRONCHIAL CONTRACTION THAT CORRELATES WITH THE RELEASE OF LEUKOTRIENE-C4, LEUKOTRIENE-D4, AND LEUKOTRIENE-E4
DAHLEN, SE
HANSSON, G
HEDQVIST, P
BJORCK, T
GRANSTROM, E
DAHLEN, B
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1983, 80 (06): : 1712 - 1716
[7] DEMONCHY JGR, 1985, AM REV RESPIR DIS, V131, P373
[8] REQUIREMENT OF A 5-LIPOXYGENASE-ACTIVATING PROTEIN FOR LEUKOTRIENE SYNTHESIS
DIXON, RAF
DIEHL, RE
OPAS, E
RANDS, E
VICKERS, PJ
EVANS, JF
GILLARD, JW
MILLER, DK
[J]. NATURE, 1990, 343 (6255) : 282 - 284
[9] GADDY J, 1990, Journal of Allergy and Clinical Immunology, V85, P197
[10] L-663,536 (MK-886) (3-[1-(4-CHLOROBENZYL)-3-T-BUTYL-THIO-5-ISOPROPYLINDOL-2-YL]-2,2-DIMETHYLPROPANOIC ACID), A NOVEL, ORALLY ACTIVE LEUKOTRIENE BIOSYNTHESIS INHIBITOR
GILLARD, J
FORDHUTCHINSON, AW
CHAN, C
CHARLESON, S
DENIS, D
FOSTER, A
FORTIN, R
LEGER, S
MCFARLANE, CS
MORTON, H
PIECHUTA, H
RIENDEAU, D
ROUZER, CA
ROKACH, J
YOUNG, R
MACINTYRE, DE
PETERSON, L
BACH, T
EIERMANN, G
HOPPLE, S
HUMES, J
HUPE, L
LUELL, S
METZGER, J
MEURER, R
MILLER, DK
OPAS, E
PACHOLOK, S
[J]. CANADIAN JOURNAL OF PHYSIOLOGY AND PHARMACOLOGY, 1989, 67 (05) : 456 - 464

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