Leukotriene B4is an indirectly acting vasoconstrictor in guinea pig aorta via an inducible type of BLT receptor

Abstract

Leukotriene B₄(LTB₄) is a potent leukocyte chemoattractant recently implicated in the pathogenesis of atherosclerosis. The aim of this study was to assess the effects of LTB₄on isolated aortic preparations. Rings of guinea pig aorta were challenged with LTB₄for recording mechanical responses and measurements of mediator release, and LTB₄receptor (BLT₁) expression was assessed by RT-PCR. Single concentrations of LTB₄induced concentration-dependent contractions that were inhibited by treatment with antihistamines, indomethacin, or the thromboxane receptor antagonist BAYu3405 as well as by denudation of endothelium. In addition, LTB₄increased the release of histamine and thromboxane in the bath. The contractions induced by LTB₄were inhibited by either the unselective BLT receptor antagonist ONO-4057 or the selective BLT₁receptor antagonist U-75302. Pretreatment with all -trans-retinoic acid enhanced the contractions and the release of histamine induced by LTB₄, without affecting either the contractions induced by histamine or the histamine release evoked by calcium ionophore A23187. Analysis by RT-PCR indicated the expression of a BLT₁receptor in the guinea pig aorta and that BLT₁receptor mRNA was upregulated after treatment with retinoic acid. These results suggest that LTB₄contracts the guinea pig aorta via an indirect mechanism involving the release of histamine and thromboxane and that this BLT₁receptor-mediated response can be upregulated by all -trans-retinoic acid.