大鼠离体灌注肾中血管P2嘌呤受体的特性研究
Characterization of vascular P2 purinoceptors in the rat isolated perfused kidney.
作者信息
Eltze M, Ullrich B
机构信息
Department of Pharmacology, Byk Gulden, Konstanz, Germany.
出版信息
Eur J Pharmacol. 1996 Jun 13;306(1-3):139-52. doi: 10.1016/0014-2999(96)00244-0.
In isolated, constant-pressure perfused rat kidneys at basal vascular tone, injected P2 purinoceptor agonists evoked vasoconstriction (alpha, beta-methylene ATP > beta, gamma-methylene ATP > ATP-gamma-S > 2-methylthio ATP > ATP > ADP = UTP). In kidneys with raised tone, the nucleotides produced vasodilatation at low doses (2-methylthio ATP > ADP = ATP = ATP-gamma-S > UTP; alpha, beta-methylene ATP and beta, gamma-methylene ATP, inactive), and constriction at high doses (alpha, beta-methylene ATP > beta, gamma-methylene ATP > ATP-gamma-S > 2-methylthio ATP > ADP = ATP > UTP). Removal of the endothelium abolished the dilator responses to the agonists. NG-Nitro-L-arginine methylester (L-NAME, 5 x 10(-5) M) abolished vasorelaxation in response to 2-methylthio ATP, a response which could be restored by additional L-arginine (3 x 10(-3) M). Both vasodilatation and constriction due to the nucleotides remained unaffected by indomethacin (3 x 10(-6) M), S-(p-nitrobenzyl)-6-thioinosine (3 x 10(-5) M) and 8-phenyltheophylline (3 x 10(-6) M). Pyridoxalphosphate-6-azophenyl-2',4'-disulphonic acid (PPADS, 1-3 x 10(-6) M), inhibited vasoconstriction caused by alpha, beta-methylene ATP, 2-methylthio ATP and UTP, but not by ATP. Suramin (3 x 10(-5) M) caused a rightward shift of the dose-response curves for constriction caused by alpha, beta-methylene ATP (27-fold) and 2-methylthio ATP (5-fold), whereas the ATP curve was shifted to the left (20-fold). With Evans blue (10(-5) M), vasodilatation due to the nucleotides was abolished and the dose-response curves for vasoconstriction caused by ATP and UTP were shifted left more than 100-fold, the effect to both could not be antagonized by PPADS (3 x 10(-6) M). These results suggest: (1) the different rank orders of P2 purinoceptor agonist potencies for constrictor and dilator responses in perfused rat kidney are consistent with mediation via P2x and P2Y purinoceptors, respectively; (2) P2X purinoceptors, selectively sensitive to blockade by PPADS, are located on vascular smooth muscle; (3) endothelial P2Y purinoceptor stimulation results in vasodilatation involving NO synthesis but not release of prostanoids; (4) Evans blue, which appears to combine selective P2Y purinoceptor blockade and strong inhibition of ecto-nucleotidases, potentiates vasoconstriction in response to the degradable nucleotides, ATP, 2-methylthio ATP and UTP; (5) additionally, Evans blue unmasks a PPADS-insensitive P2U purinoceptor where the nearly equipotent nucleotides, ATP and UTP, can produce vasoconstriction.
在基础血管张力下对分离的、恒压灌注的大鼠肾脏进行实验,注射P2嘌呤受体激动剂可引起血管收缩(α,β-亚甲基ATP > β,γ-亚甲基ATP > ATP-γ-S > 2-甲硫基ATP > ATP > ADP = UTP)。在血管张力升高的肾脏中,核苷酸在低剂量时产生血管舒张作用(2-甲硫基ATP > ADP = ATP = ATP-γ-S > UTP;α,β-亚甲基ATP和β,γ-亚甲基ATP无活性),而在高剂量时产生血管收缩作用(α,β-亚甲基ATP > β,γ-亚甲基ATP > ATP-γ-S > 2-甲硫基ATP > ADP = ATP > UTP)。去除内皮细胞可消除激动剂引起的舒张反应。NG-硝基-L-精氨酸甲酯(L-NAME,5×10⁻⁵ M)可消除对2-甲硫基ATP的血管舒张反应,额外添加L-精氨酸(3×10⁻³ M)可恢复该反应。核苷酸引起的血管舒张和收缩均不受吲哚美辛(3×10⁻⁶ M)、S-(对硝基苄基)-6-硫代肌苷(3×10⁻⁵ M)和8-苯基茶碱(3×10⁻⁶ M)的影响。磷酸吡哆醛-6-偶氮苯基-2',4'-二磺酸(PPADS,1 - 3×10⁻⁶ M)可抑制α,β-亚甲基ATP、2-甲硫基ATP和UTP引起的血管收缩,但不抑制ATP引起的血管收缩。苏拉明(3×10⁻⁵ M)使α,β-亚甲基ATP(27倍)和2-甲硫基ATP(5倍)引起的收缩剂量-反应曲线右移,而ATP曲线左移(约20倍)。使用伊文思蓝(10⁻⁵ M)后,核苷酸引起的血管舒张被消除,ATP和UTP引起的血管收缩剂量-反应曲线左移超过100倍,PPADS(3×10⁻⁶ M)无法拮抗两者的这种作用。这些结果表明:(1)灌注大鼠肾脏中P2嘌呤受体激动剂对收缩和舒张反应的不同效价顺序分别与通过P2x和P2Y嘌呤受体介导的反应一致;(2)对PPADS阻断敏感的P2X嘌呤受体位于血管平滑肌上;(3)内皮细胞P2Y嘌呤受体刺激导致血管舒张,涉及一氧化氮合成但不涉及前列腺素释放;(4)伊文思蓝似乎兼具选择性P2Y嘌呤受体阻断和对外切核苷酸酶的强烈抑制作用,可增强对可降解核苷酸ATP、2-甲硫基ATP和UTP的血管收缩反应;(5)此外,伊文思蓝揭示了一种对PPADS不敏感的P2U嘌呤受体,在此受体上,几乎等效的核苷酸ATP和UTP可产生血管收缩作用。
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