smaller in female than in male in SPZF rats, but sex differences were not observed in CP rats. Apelin mRNA levels in female CP rats were the highest among groups. The enhancements of acetylcholine-induced relaxations by PVAT were positively correlated with apelin mRNA levels in PVAT. These results demonstrated that sex difference in enhancing vasorelaxation response by PVAT in renal arteries differs to that in mesenteric arteries in SPZF rats at the same age and to that in another MetS model strain, CP rats, at the same age and arterial sites. This discrepancy observed in female rats between two MetS strains may be associated with the difference in arterial dysfunction mechanism; namely, impairment of only endothelial nitric oxide production in CP rats, and deterioration of re-sponse to nitric oxide in smooth muscle in SPZF rats. Furthermore, apelin levels of PVAT may be involved in the appearance of modulation of PVAT on arterial tone.
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