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Ro 41-1049和Ro 19-6327对A型和B型单胺氧化酶的选择性抑制对大鼠肾切片中多巴胺释放的影响。

Effect of type A and B monoamine oxidase selective inhibition by Ro 41-1049 and Ro 19-6327 on dopamine outflow in rat kidney slices.

作者信息

Pestana M, Soares-da-Silva P

机构信息

Institute of Pharmacology and Therapeutics, Faculty of Medicine, Porto, Portugal.

出版信息

Br J Pharmacol. 1994 Dec;113(4):1269-74. doi: 10.1111/j.1476-5381.1994.tb17135.x.

Abstract
  1. The influence of pargyline and of selective inhibitors of type A and B monoamine oxidase (MAO), Ro 41-1049 and Ro 19-6327 respectively, on the outflow of dopamine and 3,4-dihydroxyphenylacetic acid (DOPAC) in slices of rat renal cortex loaded with exogenous L-3,4-dihydroxyphenylalanine (L-DOPA) was examined. Dopamine and DOPAC in the tissues and in the effluent were assayed by means of h.p.l.c. with electrochemical detection. 2. The levels of newly-formed dopamine and DOPAC in the perifusate decreased progressively with time. In control conditions, DOPAC/dopamine ratios in the perifusate were 3 to 5 fold those in the tissue and were found to increase progressively with time. The addition of pargyline (100 microM), produced a marked decrease in the outflow levels of DOPAC (45 to 54% reduction) and significantly increased the levels of dopamine in the effluent (102 to 158% increase); DOPAC/dopamine ratios in the perifusate remained stable throughout the perifusion and were similar to those found in the tissues. The addition of the MAO-A inhibitor Ro 41-1049 to the perifusion fluid also significantly decreased DOPAC outflow (41% to 54% reduction) and increased dopamine outflow (19% to 80% increase). In the presence of Ro 41-1049 DOPAC/dopamine ratios in the perifusate were lower (P < 0.01) than in controls; in contrast with the effect of pargyline, this ratio was found to increase (P < 0.01) throughout the perifusion period. Ro 19-6327 did not reduce the outflow of DOPAC, but significantly increased (by 40-60%) that of dopamine. In the presence of Ro 19-6237, the proportion of DOPAC to dopamine in the perifusate was similar to that of controls and significantly increased throughout the perifusion; however, this increase was less than that observed in the control group.3. When benserazide (50 microM) was added to the perifusion fluid, the levels of both dopamine and DOPAC in the effluent were similar to those observed in the absence of benserazide. However, in the presence of benserazide, DOPAC/dopamine ratios in the perifusate did not increase with time. In conditions of decarboxylase inhibition, the effects of pargyline, Ro 41-1049 and Ro 19-6327 on dopamine and DOPAC outflow were less pronounced than in experiments conducted in the absence of benserazide.4. In conclusion, the results presented here show that the fraction of newly-formed dopamine which leaves the compartment where the synthesis has occurred is a constant source for deamination into DOPAC. The results provide evidence favouring the view that MAO-A is the main form of the enzyme involved in this process; however, the data described here suggest that dopamine would also have access to MAO-B.
摘要
  1. 分别研究了优降宁以及A型和B型单胺氧化酶(MAO)的选择性抑制剂Ro 41 - 1049和Ro 19 - 6327对加载外源性L - 3,4 - 二羟基苯丙氨酸(L - DOPA)的大鼠肾皮质切片中多巴胺和3,4 - 二羟基苯乙酸(DOPAC)流出的影响。采用高效液相色谱电化学检测法测定组织和流出液中的多巴胺和DOPAC。2. 灌注液中新生成的多巴胺和DOPAC水平随时间逐渐降低。在对照条件下,灌注液中DOPAC/多巴胺的比值是组织中的3至5倍,且发现其随时间逐渐增加。加入优降宁(100μM)后,DOPAC的流出水平显著降低(降低45%至54%),流出液中多巴胺水平显著升高(升高102%至158%);灌注液中DOPAC/多巴胺的比值在整个灌注过程中保持稳定,且与组织中的相似。向灌注液中加入MAO - A抑制剂Ro 41 - 1049也显著降低了DOPAC的流出(降低41%至54%),并增加了多巴胺的流出(增加19%至80%)。在Ro 41 - 1049存在的情况下,灌注液中DOPAC/多巴胺的比值低于对照组(P < 0.01);与优降宁的作用相反,该比值在整个灌注期间增加(P < 0.01)。Ro 19 - 6327没有降低DOPAC的流出,但显著增加了(40 - 60%)多巴胺的流出。在Ro 19 - 6237存在的情况下,灌注液中DOPAC与多巴胺的比例与对照组相似,且在整个灌注过程中显著增加;然而,这种增加小于对照组中观察到的增加。3. 当向灌注液中加入苄丝肼(50μM)时,流出液中多巴胺和DOPAC水平与未加入苄丝肼时观察到的相似。然而,在苄丝肼存在的情况下,灌注液中DOPAC/多巴胺的比值不会随时间增加。在脱羧酶抑制的条件下,优降宁、Ro 41 - 1049和Ro 19 - 6327对多巴胺和DOPAC流出的影响不如在未加入苄丝肼的实验中明显。4. 总之,此处给出的结果表明,离开合成发生部位的新生成多巴胺部分是脱氨基生成DOPAC的恒定来源。这些结果为支持MAO - A是参与此过程的主要酶形式这一观点提供了证据;然而,此处描述的数据表明多巴胺也可接触到MAO - B。

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本文引用的文献

7
Evidence that intrarenal dopamine acts as a paracrine substance at the renal tubule.
Am J Physiol. 1989 Sep;257(3 Pt 2):F469-77. doi: 10.1152/ajprenal.1989.257.3.F469.
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Evidence for an extraneuronal location of monoamine oxidase in renal tissues.
Naunyn Schmiedebergs Arch Pharmacol. 1990 May;341(5):411-3. doi: 10.1007/BF00176332.

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