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人输尿管中环核苷酸磷酸二酯酶同工酶的特性及其体外功能作用

Characterization of cyclic nucleotide phosphodiesterase isoenzymes in the human ureter and their functional role in vitro.

作者信息

Taher A, Schulz-Knappe P, Meyer M, Truss M, Forssmann W G, Stief C G, Jonas U

机构信息

Department of Urology, Medical School, Hannover, Germany.

出版信息

World J Urol. 1994;12(5):286-91. doi: 10.1007/BF00191209.

DOI:10.1007/BF00191209
PMID:7866426
Abstract

An increase in cyclic nucleotide monophosphate levels is suggested to play a prominent role in mediating smooth-muscle relaxation. Cyclic nucleotide phosphodiesterase (PDE) influences smooth-muscle tone by decreasing the level of cyclic nucleotides. At present, five different families of isoenzymes of PDE exist that show a distinct species- and organ-specific distribution. Our study was done to evaluate the existence of specific PDE isoenzymes and its functional role in human ureteral tissue. Normal ureteral tissue was homogenized and centrifuged and the supernatant fraction was separated using anioin-exchange diethylaminoethyl (DEAE)-Sephacel chromatography. A PDE assay was then performed and the peak fractions were added to different specific PDE activators and inhibitors. In vitro, longitudinal ureteral strips were precontracted and different selective and non-selective PDE inhibitors were added incremently. Three different PDE isoenzymes were characterized: PDE I (calmodulin-sensitive), PDE II (cGMP-stimulated), and PDE IV (cAMP-specific). All PDE inhibitors relaxed the strips dose-dependently, with the 50% effective concentrations (EC50) being 30 microM for papaverine, 40 microM for zaprinast, 25 microM for quazinone, and 0.1 microM for rolipram. The ureter-relaxing effect of the PDE IV inhibitor at low concentrations, combined with its low-level effect on the systemic circulatory parameters, may open the possibility of using selective PDE IV-inhibitors in the treatment of ureteral colics or for ureteral stone passage.

摘要

环磷酸核苷酸水平的升高被认为在介导平滑肌舒张中起重要作用。环磷酸核苷酸磷酸二酯酶(PDE)通过降低环磷酸核苷酸水平来影响平滑肌张力。目前,存在五种不同的PDE同工酶家族,它们表现出明显的物种和器官特异性分布。我们的研究旨在评估特异性PDE同工酶在人输尿管组织中的存在及其功能作用。将正常输尿管组织匀浆并离心,然后使用阴离子交换二乙氨基乙基(DEAE)-Sephacel色谱法分离上清液部分。接着进行PDE测定,并将峰值部分添加到不同的特异性PDE激活剂和抑制剂中。在体外,将输尿管纵行条预先收缩,然后递增添加不同的选择性和非选择性PDE抑制剂。鉴定出三种不同的PDE同工酶:PDE I(钙调蛋白敏感型)、PDE II(cGMP刺激型)和PDE IV(cAMP特异性)。所有PDE抑制剂均能剂量依赖性地舒张条带,罂粟碱的50%有效浓度(EC50)为30 microM,扎普司特为40 microM,喹齐酮为25 microM,咯利普兰为0.1 microM。PDE IV抑制剂在低浓度时的输尿管舒张作用,及其对全身循环参数的低水平影响,可能为在输尿管绞痛治疗或输尿管结石排出中使用选择性PDE IV抑制剂开辟了可能性。

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