Rasmussen J B, Eriksson L O, Margolskee D J, Tagari P, Williams V C, Andersson K E
Department of Pulmonary Medicine, Malmö General Hospital, Sweden.
J Allergy Clin Immunol. 1992 Aug;90(2):193-201. doi: 10.1016/0091-6749(92)90071-9.
We have tested the hypothesis that leukotriene D4 (LTD4) receptor activation is involved in the development of antigen-induced bronchoconstriction. In two studies, patients with asthma received infusions of placebo or MK-571, a potent and specific LTD4 receptor antagonist (450 mg or 37.5 mg total dose, respectively). Antigen was inhaled during test-drug administration, and FEV1 was measured for 10 hours after challenge. Urine samples were collected for measurement of LTE4; plasma samples were drawn repeatedly for assay of MK-571. MK-571 infusions inhibited both immediate (0 to 3 hours) and late (3 to 10 hours) asthmatic responses. For the high MK-571 dose, the extent of inhibition, as assessed by the area under the curve of FEV1 versus time was 88% (p = 0.01) and 63% (p = 0.01), for immediate and late responses, respectively. The low MK-571 dose also inhibited both responses but to a minor extent. Mean urinary LTE4 excretion was elevated after antigen challenge and was unaffected by administration of the LTD4 receptor antagonist. The present study demonstrates that MK-571 inhibits antigen-induced asthma in a dose-related fashion; it had not effect on antigen-induced increases in urinary LTE4 excretions. The results suggest that LTD4 receptor activation plays an important role in antigen-induced asthma.
我们检验了白三烯D4(LTD4)受体激活参与抗原诱导的支气管收缩发展过程这一假说。在两项研究中,哮喘患者接受安慰剂或MK-571(一种强效且特异性的LTD4受体拮抗剂,总剂量分别为450毫克或37.5毫克)输注。在给予试验药物期间吸入抗原,并在激发后10小时测量第一秒用力呼气量(FEV1)。收集尿液样本以测量LTE4;反复采集血浆样本以测定MK-571。MK-571输注抑制了即刻(0至3小时)和迟发(3至10小时)哮喘反应。对于高剂量MK-571,通过FEV1与时间曲线下面积评估的抑制程度,即刻反应和迟发反应分别为88%(p = 0.01)和63%(p = 0.01)。低剂量MK-571也抑制了两种反应,但程度较小。抗原激发后尿LTE4平均排泄量升高,且不受LTD4受体拮抗剂给药的影响。本研究表明,MK-571以剂量相关方式抑制抗原诱导的哮喘;它对抗原诱导的尿LTE4排泄增加没有影响。结果提示,LTD4受体激活在抗原诱导的哮喘中起重要作用。
