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01); the pD2 values for the regional cardiac I/R model and sham rings were not significantly different (1.50 �� 0.08 and 1.57 �� 0.04; Fig. 2A). Cardiac I/R resulted in increased vasoconstriction induced by PE in the mesenteric arterial rings, and the concentration�Cresponse curves shifted towards the left?versus?the sham group. The?Emax values for the regional cardiac I/R model were increased from 88 �� 10 to 127 �� 6% (sham?versus?I/R, respectively;?P?Selleckchem C59 wnt to U46619, a thromboxane A2 receptor agonist (9,11-dideoxy-11��,9��-epoxy-methanoprostaglandin F2��), compared with those from the sham-operated group. Likewise,?Emax (223 �� 18%) was enhanced when compared with the sham group (150 �� 20%;?P?MAO when compared with the sham group (114 �� 21%;?P? curves to PE were repeated after pretreatment with the non-selective nitric-oxide synthase inhibitor l-NAME (100 ��m) for 30 min. Significant changes as a result of l-NAME pretreatment would reveal effects of basal NO availability or production on contraction. As shown in Fig. 3A?and?B, l-NAME abolished the differences between the sham group (147 �� 11%) and the I/R group (149 �� 12%;?P?> 0.05). The change in contraction after l-NAME pretreatment was significantly greater in the sham group compared with the I/R group. We also investigated endothelium-dependent and endothelium-independent vasodilatation of rat mesenteric Selleck SP600125 arteries after regional cardiac I/R. Vasodilatation was induced by the endothelium-independent vasodilator SNP (1 �� 10?10 to 1 �� 10?6 mol l?1) and the endothelium-dependent vasodilator ACh (1 �� 10?11 to 1 �� 10?4 mol l?1). Relaxation in response to ACh was significantly reduced in PE-precontracted mesenteric segments after cardiac I/R compared with the sham group. The?Emax and pD2 values of arterial rings in the regional cardiac I/R model (65 �� 6% and 8.07 �� 0.26, respectively) were lower than those of their respective control (86 �� 6% and 8.49 �� 0.19, respectively;?P?