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Human Isolated Coronary Artery Contraction to Sumatriptan Characterised by the Selective 5‐HT 1B/1D Receptor Antagonist GR55562
Author(s) -
MaassenVanDenBrink Antoinette,
Reekers Marije,
Bax Willem A.,
Saxena Pramod R.
Publication year - 2000
Publication title -
pharmacology & toxicology
Language(s) - English
Resource type - Journals
eISSN - 1600-0773
pISSN - 0901-9928
DOI - 10.1111/j.0901-9928.2000.860608.x
Subject(s) - sumatriptan , antagonist , contraction (grammar) , receptor antagonist , 5 ht receptor , pharmacology , medicine , receptor , cardiology , chemistry , anesthesia , serotonin , agonist
The antimigraine drug, sumatriptan, contracts the human coronary artery both in vivo and in vitro. Because sumatriptan has been associated with cardiac side effects, it is important to characterise the receptor involved in sumatriptan‐induced coronary artery contraction. Using the agonists sumatriptan and 5‐carboxamidotryptamine and the selective 5‐HT 1B/1D receptor antagonist GR55562, we have investigated the involvement of 5‐HT 1B/1D receptors in the contraction of the human isolated coronary artery. Contractions to sumatriptan (pEC 50 : 6.1±0.2, maximal effect: 21±4% of 100 mM K + ‐induced contraction) were competitively antagonised by GR55562. The pA 2 of GR55562 (7.40±0.16) was in accord with its reported affinity at the human 5‐HT 1B receptor. Since the contractions to 5‐carboxamidotryptamine did not reach a maximum with the highest concentration used (10 μM), pEC 50 values could not be calculated for Schild analysis. However, using the pEC 10%K+ values (negative logarithm of the concentration needed to induce 10% of the contraction to 100 mM K + ), GR55562 proved a less potent antagonist against 5‐carboxamidotryptamine than against sumatriptan. These results show that sumatriptan contracts the human isolated coronary artery via 5‐HT 1B/1D receptors, most probably the 5‐HT 1B subtype. 5‐Carboxamidotryptamine may contract the human isolated coronary artery, at least partly, via a novel yet to be characterised, receptor.

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