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克罗卡林和平尼地尔对豚鼠膀胱平滑肌86Rb外流的影响。

Effect of cromakalim and pinacidil on 86Rb efflux from guinea pig urinary bladder smooth muscle.

作者信息

Trivedi S, Stetz S, Levin R, Li J, Kau S

机构信息

Department of Pharmacology, Zeneca Pharmaceuticals Group, Zeneca Inc., Wilmington, Del 19897.

出版信息

Pharmacology. 1994 Sep;49(3):159-66. doi: 10.1159/000139230.

Abstract

86Rb efflux assay was used to investigate the effect of cromakalim, pinacidil and P1075 in guinea pig urinary bladder strips. The type of K channel opened by cromakalim and pinacidil was determined using specific K channel blockers through 86Rb efflux assay in detrusor strips. Cromakalim, pinacidil and P1075 all three potassium channel openers (PCOs) evoked a concentration-dependent increase in 86Rb efflux in bladder strips. This increase in isotope release was inhibited by pretreatment of bladder with 10 and 30 microM glibenclamide suggesting that both cromakalim and pinacidil interact with ATP-sensitive K channels (KATP). Further, an increase in basal 86Rb efflux was observed when 2-deoxy-D-glucose was substituted for glucose together with 0.24 micrograms/ml of oligomycin (known to lower intracellular ATP) indicating the presence of KATP channels in bladder smooth muscle. Charybdotoxin and apamin, blockers of large and small conductance Ca(2+)-dependent K channels, were found not to be involved in the action of these PCOs in bladder strips. alpha-Dendrotoxin, known to block voltage-dependent K channels, slightly reduced pinacidil-induced 86Rb release without affecting cromakalim-induced 86Rb efflux. The present studies show that ATP-sensitive K channels are present in guinea pig urinary bladder and that cromakalim and pinacidil act by opening these ATP-sensitive K channels in detrusor strips.

摘要

采用⁸⁶Rb外流试验研究了克罗卡林、吡那地尔和P1075对豚鼠膀胱条的作用。通过在逼尿肌条上进行⁸⁶Rb外流试验,使用特异性钾通道阻滞剂确定了克罗卡林和吡那地尔所开启的钾通道类型。克罗卡林、吡那地尔和P1075这三种钾通道开放剂(PCOs)均引起膀胱条中⁸⁶Rb外流呈浓度依赖性增加。用10和30微摩尔格列本脲预处理膀胱可抑制这种同位素释放的增加,这表明克罗卡林和吡那地尔均与ATP敏感性钾通道(KATP)相互作用。此外,当用2-脱氧-D-葡萄糖替代葡萄糖并加入0.24微克/毫升寡霉素(已知可降低细胞内ATP)时,观察到基础⁸⁶Rb外流增加,这表明膀胱平滑肌中存在KATP通道。发现大电导和小电导钙依赖性钾通道的阻滞剂蝎毒素和蜂毒肽不参与这些PCOs对膀胱条的作用。已知可阻断电压依赖性钾通道的α-树眼镜蛇毒素可轻微降低吡那地尔诱导的⁸⁶Rb释放,但不影响克罗卡林诱导的⁸⁶Rb外流。本研究表明,豚鼠膀胱中存在ATP敏感性钾通道,克罗卡林和吡那地尔通过在逼尿肌条中开启这些ATP敏感性钾通道发挥作用。

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