Pharmacomodulation Studies of Torasemide Leading to Original Non‐carboxylic Thromboxane A2 Receptor Antagonists

Pharmacy and Pharmacology Communications Pub Date : 2000-02-01 DOI:10.1211/146080800128735674

J. Dogné, X. Leval, P. Neven, S. Rolin, J. Wouters, J. Delarge, B. Masereel

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Abstract

Because torasemide, a loop diuretic, dose-dependently relaxes canine coronary artery precontracted with thromboxane A2 (TxA2), a series of pyridine derivatives have been investigated with the aim of developing original TxA2 receptor antagonists. A binding test showed the affinity (IC50; the dose reducing binding by 50%) of one sulphonylurea derivative (BM 27) and two sulphonylcyanoguanidine derivatives (BM 114 and BM 115) for the TxA2 receptor of washed platelets from man were 161, 1. 75 and 0.54 μM, respectively. The IC50 of torasemide was only 2.69 μM. Their antagonism was confirmed by the capacity of the compounds to prevent the aggregation of platelets, from man, induced by arachidonic acid, the biological precursor of TxA2 (IC50: BM 114, 29.3 μM; BM 115, 12.0 μM; BM 27, 234 μM; torasemide, 350 μM; sulotroban, 12.3 μM). Similar results were obtained with the best compound BM 115 (IC50 11.5 μM) when U-46619, a stable TxA2 agonist, was used as the aggregating agent. This molecule can be regarded as a template for the design of novel non-carboxylic TxA2 receptor antagonists.

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托拉塞米导致原始非羧基血栓素A2受体拮抗剂的药物调节研究

由于torasemide是一种环形利尿剂，剂量依赖性地放松犬冠状动脉血栓素A2 (TxA2)的预收缩，一系列吡啶衍生物已被研究，目的是开发原始的TxA2受体拮抗剂。结合试验显示亲和性(IC50;一种磺脲类衍生物(bm27)和两种磺酰基氰基胍类衍生物(bm114和bm115)与人洗涤血小板TxA2受体的结合剂量降低50%(161,1)。0.75 μM, 0.54 μM。托拉塞米的IC50仅为2.69 μM。它们的拮抗作用被证实是通过抑制花生四烯酸诱导的血小板聚集，花生四烯酸是TxA2的生物前体(IC50: BM 114, 29.3 μM;Bm 115, 12.0 μm;Bm 27,234 μm;torasemide, 350 μM;sulotroban, 12.3 μM)。以稳定的TxA2激动剂U-46619为聚集剂，最佳化合物bm115 (IC50为11.5 μM)得到了相似的结果。该分子可作为设计新型非羧基TxA2受体拮抗剂的模板。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Pharmacy and Pharmacology Communications

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