SELECTIVE INHIBITORY ACTIONS OF SODIUM‐p‐BENZYL‐4‐[1‐OXO‐2‐(4‐CHLOROBENZYL)‐3‐PHENYL PROPYL] PHENYL PHOSPHONATE (N‐O164) AND INDOMETHACIN ON THE BIOSYNTHESIS OF PROSTAGLANDINS AND THROMBOXANES FROM ARACHIDONIC ACID
Open Access
- 1 May 1977
- journal article
- Published by Wiley in British Journal of Pharmacology
- Vol. 60 (1) , 135-140
- https://doi.org/10.1111/j.1476-5381.1977.tb16757.x
Abstract
1 Sodium p-benzyl-4-[1-oxo-2-(4-chlorobenzyl)-3-phenyl propyl]phenyl phosphonate (N-0164) selectively inhibited the formation of thromboxane-A2 from prostaglandin endoperoxides by human platelet microsomes in a dose-dependent manner (IC50 2.2 × 10−5 m or 11.6 μg/ml). 2 N-0164 was approximately 15 to 20 times as potent as indomethacin as an inhibitor of thromboxane-A2 formation. In contrast, indomethacin was 20 times as potent as N-0164 as an inhibitor of prostaglandin endoperoxide formation from arachidonic acid (IC50 2.6 × 10−5 m or 9.4 μg/ml). 3 Spiral strips of dog coronary arteries relaxed in the presence of prostaglandin endoperoxides and were contracted by prostaglandin E2 and thromboxane-A2 and were therefore used to distinguish between prostaglandins and their intermediate precursors, the endoperoxides. 4 Neither indomethacin nor N-0164 (both 50 μg/ml) significantly inhibited the formation of prostaglandin-like activity from the endoperoxides following incubation with indomethacin-pretreated rabbit kidney medulla microsomes. 5 It is not known whether this action of N-0164 is related to its ability to antagonize certain actions of prostaglandins (and related compounds) or whether N-0164 can penetrate the cell membrane to inhibit thromboxane formation in the intact cell. 6 Selective inhibition of thromboxane formation by drugs such as N-0164 may be useful both clinically and as a pharmacological tool to elucidate the patho-physiological roles of the thromboxanes.Keywords
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