Dihydroergotamine and sumatriptan in isolated human coronary artery, middle meningeal artery and saphenous vein

Dihydroergotamine and sumatriptan in isolated human coronary artery, middle meningeal artery and saphenous vein

Dihydroergotamine (DHE) and sumatriptan are contraindicated in patients with cardiovascular disease because of their vasoconstricting properties, which have originally been explored in proximal coronary arteries. Our aim was to investigate DHE and sumatriptan in the proximal and distal coronary arte...

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Bibliographic Details
Published in:Cephalalgia Vol. 35; no. 2; p. 182
Main Authors: Labruijere, Sieneke, Chan, Kayi Y, de Vries, René, van den Bogaerdt, Antoon J, Dirven, Clemens M, Danser, Ah Jan, Kori, Shashidhar H, MaassenVanDenBrink, Antoinette
Format: Journal Article
Language:English
Published: England 01-02-2015
Subjects:
Adolescent
Adult
Aged
Coronary Vessels - drug effects
Dihydroergotamine - pharmacology
Female
Humans
Male
Meningeal Arteries - drug effects
Middle Aged
Organ Culture Techniques
Saphenous Vein - drug effects
Sumatriptan - pharmacology
Vasoconstriction - drug effects
Vasoconstrictor Agents - pharmacology
Young Adult
vasoconstriction
5-HT
dihydroergotamine
Migraine
human coronary artery
sumatriptan
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Summary:Dihydroergotamine (DHE) and sumatriptan are contraindicated in patients with cardiovascular disease because of their vasoconstricting properties, which have originally been explored in proximal coronary arteries. Our aim was to investigate DHE and sumatriptan in the proximal and distal coronary artery, middle meningeal artery and saphenous vein. Blood vessel segments were mounted in organ baths and concentration response curves for DHE and sumatriptan were constructed. In the proximal coronary artery, meningeal artery and saphenous vein, maximal contractions to DHE (proximal: 8 ± 4%; meningeal: 32 ± 7%; saphenous: 52 ± 11%) and sumatriptan (proximal: 17 ± 7%; meningeal: 61 ± 18%, saphenous: 37 ± 8%) were not significantly different. In the distal coronary artery, contractions to DHE (5 ± 2%) were significantly smaller than those to sumatriptan (17 ± 9%). At clinically relevant concentrations, mean contractions to DHE and sumatriptan were below 3% in proximal coronary arteries and below 6% in distal coronary arteries. Contractions in the meningeal artery and saphenous vein were higher (7%-38%). Contractions to DHE in distal coronary arteries are smaller than those to sumatriptan, while at clinical concentrations they both induce only slight contractions. In meningeal arteries contractions to DHE and sumatriptan are significantly larger, showing their cranioselectivity. Contractions to DHE in the saphenous vein are higher than those in the arteries, confirming its venous contractile properties.
ISSN:1468-2982
DOI:10.1177/0333102414544977