Goldie R G, Paterson J W
Br J Pharmacol. 1982 Aug;76(4):507-13. doi: 10.1111/j.1476-5381.1982.tb09247.x.
1 Lung parenchyma strips of the pig incubated at 37 degrees C with [(3)H]-(-)-noradrenaline ([(3)H]-NA) or [(3)H]-(+/-)-isoprenaline ([(3)H]-Iso), accumulated radioactivity via saturable, high affinity uptake processes. Apparent saturation constants (K(m)) for [(3)H]-NA and [(3)H]-Iso were 1.34 x 10(-6) M and 1.63 x 10(-6) M respectively, while apparent transport maxima (V(max)) were 4.86 and 1.63 x 10(-9) mol min(-1) g(-1) respectively.2 Cellular accumulation of radioactivity from radiolabelled catecholamines was greatly reduced by lowering the temperature to 7 degrees C, pretreatment with ouabain (100 muM), phentolamine (15 muM) or phenoxybenzamine (80 muM). However, accumulation of radioactivity derived from ((3)H]-NA was inhibited selectively by cocaine (10 muM) and desipramine (1 muM), while normetanephrine (80 muM) and 3-O-methylisoprenaline (50 muM) caused much greater reductions in cellular radioactivity from [(3)H]-Iso than from ((3)H]-NA. Taken together with information from kinetic studies, the results indicate that these amines are transported by separate uptake processes.3 Cocaine (50 muM) which selectively reduced [(3)H]-NA transport, had no significant effect on the sensitivity (EC(50)) of isolated parenchyma lung strips of the pig to the contractile effects of cumulative concentrations of NA. The catechol-O-methyl transferase (COMT) inhibitor, U-0521 (60 muM), also failed to alter the potency of NA, while normetanephrine (80 muM) caused a 2 fold decrease in potency.4 Phentolamine (15 muM), which reduced the cellular accumulation of radioactivity derived from [(3)H]-Iso by 64%, caused a small potentiation of Iso-induced relaxations of porcine lung strips. Normetanephrine (80 muM) and 3-O-methylisoprenaline (50 muM), which also depressed the accumulation of cellular radioactivity from [(3)H]-Iso by > 50%, caused rightward shifts in Iso concentration-effect curves as a result of beta-adrenoceptor blockade. In sharp contrast, cortisol (80 muM) and U-0521 (60 muM), which caused smaller reductions in the cellular accumulation of radioactivity derived from [(3)H]-Iso, both caused an approximately 9 fold potentiation of responses to Iso in isolated lung strips.5 The results indicate that the major sites of uptake and metabolism of NA in porcine parenchyma strip are remote from alpha-adrenoceptors mediating NA-induced contraction. Similarly, some major sites of uptake of Iso are remote from beta-adrenoceptors mediating Iso-induced relaxation. However, beta-adrenoceptors are apparently in close proximity to a compartment containing COMT activity.
将猪的肺实质条带在37℃下与[³H]-(-)-去甲肾上腺素([³H]-NA)或[³H]-(±)-异丙肾上腺素([³H]-Iso)一起孵育,通过可饱和的高亲和力摄取过程积累放射性。[³H]-NA和[³H]-Iso的表观饱和常数(Kₘ)分别为1.34×10⁻⁶M和1.63×10⁻⁶M,而表观转运最大值(Vₘₐₓ)分别为4.86和1.63×10⁻⁹mol·min⁻¹·g⁻¹。
通过将温度降至7℃、用哇巴因(100μM)、酚妥拉明(15μM)或酚苄明(80μM)预处理,放射性标记的儿茶酚胺的细胞内放射性积累大大减少。然而,可卡因(10μM)和地昔帕明(1μM)选择性抑制了源自[³H]-NA的放射性积累,而去甲变肾上腺素(80μM)和3 - O - 甲基异丙肾上腺素(50μM)对[³H]-Iso的细胞内放射性的降低作用比对[³H]-NA的作用大得多。结合动力学研究的信息,结果表明这些胺通过不同的摄取过程进行转运。
选择性降低[³H]-NA转运的可卡因(50μM)对猪离体肺实质条带对累积浓度的NA收缩作用的敏感性(EC₅₀)没有显著影响。儿茶酚 - O - 甲基转移酶(COMT)抑制剂U - 0521(60μM)也未能改变NA的效力,而去甲变肾上腺素(80μM)使效力降低了2倍。
酚妥拉明(15μM)使源自[³H]-Iso的放射性细胞内积累减少了64%,导致异丙肾上腺素诱导的猪肺条带舒张有小的增强作用。去甲变肾上腺素(80μM)和3 - O - 甲基异丙肾上腺素(50μM)也使源自[³H]-Iso的细胞内放射性积累降低>50%,由于β - 肾上腺素能受体阻断,导致异丙肾上腺素浓度 - 效应曲线右移。形成鲜明对比的是,皮质醇(80μM)和U - 0521(60μM)使源自[³H]-Iso的放射性细胞内积累减少较小,但两者都使离体肺条带对异丙肾上腺素的反应增强约9倍。
结果表明,猪肺实质条带中去甲肾上腺素摄取和代谢的主要部位远离介导去甲肾上腺素诱导收缩的α - 肾上腺素能受体。同样,异丙肾上腺素摄取的一些主要部位远离介导异丙肾上腺素诱导舒张的β - 肾上腺素能受体。然而,β - 肾上腺素能受体显然紧邻含有COMT活性的区室。
