Vascular responses to leukotriene B4, C4 and D4 following FPL 55712, indomethacin, saralasin, phentolamine and verapamil in the conscious rat

Abstract

The pressor and vascular permeability effects of leukotrienes B₄ (LTB₄), C₄ and D₄ were investigated in conscious unrestrained rats. Leukotrienes C₄ and D₄ (3.2–51 nmol kg⁻¹ i.v.) caused an acute dose‐dependent elevation of the mean arterial pressure, which was maximal after 2 min and returned to control levels within 14 min. Heart rate was significantly reduced by the higher doses of LTC₄ and LTD₄. LTB₄ (up to a dose of 51 nmol kg⁻¹) was essentially inactive. These effects of LTC₄ and LTD₄ were abolished by FPL 55712, a putative antagonist of sulphidopeptide leukotrienes and by verapamil, a calcium channel blocker. Indomethacin, phentolamine or saralasin pretreatment failed to modify the pressor response to LTC₄ and LTD₄. LTC₄ and LTD₄ furthermore caused an increase in haematocrit values, which was significantly attenuated by FPL 55712, indomethacin and verapamil. The present findings show that the pressor effect of LTC₄ and LTD₄ is not related to prostanoid release and can be reversed by calcium channel blockade; whereas the effect on vascular permeability seems to require the presence of both cyclo‐oxygenase product(s) and calcium.