Lack of Endotoxin-lnduced Hyporesponsiveness to U46619 in Isolated Neonatal Porcine Pulmonary but Not Mesenteric Arteries

Abstract

The effects of endotoxin from Escherichia coli on the vasoconstrictor responses to noradrenaline (10 nM–100 µM) and the thromboxane A₂ analog U46619 (100 pM–1 µM) were evaluated on isolated pulmonary and mesenteric arteries from neonatal piglets. Incubation for 20 h with endotoxin (1 µg ml^–1) induced a decrease in the contractile responses to noradrenaline in both arteries (p G-nitro-L-arginine-methyl ester (L-NAME, 100 µM). Endotoxin-treated mesenteric arteries also showed a reduction of the maximal contractions induced by U46619 (p L-NAME. In contrast, the contractile responses to U46619 were similar in control and endotoxin-treated pulmonary arteries. In endothelium-denuded pulmonary rings, endotoxin was also unable to modify the contractile responses to U46619. In pulmonary rings, the contractions induced by U46619 (100 nM) were much less sensitive to sodium nitroprus-side, 8-bromo-cyclic GMP or dipyridamole than those induced by 10 µM noradrenaline. In conclusion, endotoxin-treated pulmonary arteries exhibited decreased responses to noradrenaline due to enhanced nitric oxide release but not to the thromboxane A₂ analog U46619. This lack of hyporesponsiveness to U46619 in pulmonary arteries may be attributed to a relative insensitivity to nitric oxide. The absence of pulmonary hyporesponsiveness to U46619 may explain why pulmonary hypertension occurs in septic shock despite Ca²⁺-inde-pendent nitric oxide synthase induction in the lung.