SK&F S - 106203抑制清醒大鼠体内白三烯C4、白三烯D4和白三烯E4的升压反应。

SK&F S-106203 inhibits leukotriene C4, leukotriene D4 and leukotriene E4 vasopressor responses in the conscious rat.

作者信息

Smith E F, Slivjak M J, Egan J W, Eckardt R D, Newton J F

机构信息

SmithKline Beecham Pharmaceuticals plc, Department of Pharmacology, King of Prussia, PA 19406.

出版信息

Br J Pharmacol. 1990 Jun;100(2):195-200. doi: 10.1111/j.1476-5381.1990.tb15781.x.

DOI:10.1111/j.1476-5381.1990.tb15781.x

PMID:2165834

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1917428/

Abstract

The purpose of these experiments was to investigate the effects of the selective peptidoleukotriene receptor antagonist, SK&F S-106203, on leukotriene C4 (LTC4), LTD4 and LTE4 vasopressor responses in the conscious, normotensive rat. SK&F S-106203 was administered as a bolus followed by a continuous infusion in order to provide information on the relationship between antagonism of leukotriene responses and steady-state plasma concentrations. 2. Infusion of SK&F S-106203 at doses of 0.2 mgkg-1 + 1 mgkg-1 h-1, 1 mgkg-1 + 3 mgkg- h-1 or 2 mgkg-1 + 10 mgkg-1 h-1 produced dose-dependent steady-state plasma drug concentrations of 1.0, 3.2 and 23.8 micrograms ml-1, respectively. Plasma SK&F S-106203 concentrations appeared to increase in a linear fashion at doses of 1 and 3 mgkg-1 h-1; at the highest dose the increment in plasma drug concentrations (i.e., 7-8 fold) was greater than the increment in dose (i.e., 3 fold), suggesting saturation of the primary clearance mechanism(s) at this dose. 3. SK&F S-106203 (2 mgkg-1 + 10 mgkg-1 h-1) had no effect on noradrenaline-, vasopressin-, isoprenaline-, or U 46619-induced responses. 4. SK&F S-106203 produced dose-dependent rightward shifts in the LTC4 and LTE4 dose-response curves. Administration of SK&F S-106203 at doses of 0.2mg kg1 + 1 mg kg1 h-, mg kg' + 3mgkg-'h-1, or 2mgkg-' + lOmgkg-1h'- produced dose-ratios of 1.0, 3.1 and 19.9, respectively, against LTC4 responses, and dose-ratios of 1.6, 3.8 and 9.1, respectively, against LTE4 responses. 5. Against LTD4 responses, SK&F S-106203 at doses of 0.2mgkg- + mgkg-1 h-, mg kg' + 3 mg kg- 1h - ', or 2 mg kg- + 10 mg kg- h- produced dose-ratios of 2.5, 2.8, and 11.4, respectively. Administration of D-penicillamine, a non-competitive LTD4 dipeptidase inhibitor, had no effect on LTD4 responses. 6. The similarity in the LTD4 dose-ratios at the two lower infusion rates, despite increases in the plasma drug concentrations, suggests the existence of pharmacologically heterogeneous LTD4 receptors. These results indicate that SK&F S-106203 is a potent, selective and apparently competitive antagonist of LTC4, LTD4 and LTE4 vascular responses in the intact rat.

摘要

这些实验的目的是研究选择性肽白三烯受体拮抗剂SK&F S - 106203对清醒、血压正常大鼠体内白三烯C4（LTC4）、白三烯D4（LTD4）和白三烯E4（LTE4）升压反应的影响。SK&F S - 106203以推注给药，随后持续输注，以提供有关白三烯反应拮抗作用与稳态血浆浓度之间关系的信息。2. 以0.2mgkg-1 + 1mgkg-1 h-1、1mgkg-1 + 3mgkg-1 h-1或2mgkg-1 + 10mgkg-1 h-1的剂量输注SK&F S - 106203，分别产生剂量依赖性的稳态血浆药物浓度1.0、3.2和23.8微克/毫升。在1和3mgkg-1 h-1的剂量下，血浆SK&F S - 106203浓度似乎呈线性增加；在最高剂量下，血浆药物浓度的增加（即7 - 8倍）大于剂量的增加（即3倍），表明该剂量下主要清除机制出现饱和。3. SK&F S - 106203（2mgkg-1 + 10mgkg-1 h-1）对去甲肾上腺素、血管加压素、异丙肾上腺素或U 46619诱导的反应无影响。4. SK&F S - 106203使LTC4和LTE4剂量反应曲线产生剂量依赖性的右移。以0.2mg kg-1 + 1mg kg-1 h-1、1mg kg-1 + 3mgkg-1 h-1或2mgkg-1 + 10mgkg-1 h-1的剂量给药SK&F S - 106203，对LTC4反应的剂量比分别为1.0、3.1和19.9，对LTE4反应的剂量比分别为1.6、3.8和9.1。5. 对于LTD4反应，以0.2mgkg-1 + 1mgkg-1 h-1、1mg kg-1 + 3mg kg-1 h-1或2mg kg-1 + 10mg kg-1 h-1的剂量给药SK&F S - 106203，剂量比分别为2.5、2.8和11.4。给予非竞争性LTD4二肽酶抑制剂D - 青霉胺对LTD4反应无影响。6. 尽管血浆药物浓度增加，但在两个较低输注速率下LTD4剂量比相似，这表明存在药理学上异质性的LTD4受体。这些结果表明，SK&F S - 106203是完整大鼠体内LTC4、LTD4和LTE4血管反应的强效、选择性且明显具有竞争性的拮抗剂。