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Physiological significance of P2X receptor-mediated vasoconstriction in five different types of arteries in rats
[摘要] P2X1 receptors, the major subtype of P2X receptors in the vascular smooth muscle, are essential for α,β-methylene adenosine 5′-triphosphate (α,β-MeATP)-induced vasoconstriction. However, relative physiological significance of P2X1 receptor-regulated vasoconstriction in the different types of arteries in the rat is not clear as compared with α1-adrenoceptor-regulated vasoconstriction. In the present study, we found that vasoconstrictive responses to noncumulative administration of α,β-MeATP in the rat isolated mesenteric arteries were significantly smaller than those to single concentration administration of α,β-MeATP. Therefore, we firstly reported the characteristic of α,β-MeATP-regulated vasoconstrictions in rat tail, internal carotid, pulmonary, mesenteric arteries, and aorta using single concentration administration of α,β-MeATP. The rank order of maximal vasoconstrictions for α,β-MeATP (Emax·α,β-MeATP) was the same as that of maximal vasoconstrictions for noradrenaline (Emax·NA) in the internal carotid, pulmonary, mesenteric arteries, and aorta. Moreover, the value of (Emax·α,β-MeATP/Emax·KCl)/(Emax·NA/Emax·KCl) was 0.4 in each of the four arteries, but it was 0.8 in the tail artery. In conclusion, P2X1 receptor-mediated vasoconstrictions are equally important in rat internal carotid, pulmonary, mesenteric arteries, and aorta, but much greater in the tail artery, suggesting its special role in physiological function.

[发布日期]  [发布机构] 
[效力级别]  [学科分类] 分子生物学,细胞生物学和基因
[关键词] Rat [时效性] 
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