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环核苷酸在豚鼠膀胱收缩性中的作用。

The role of cyclic nucleotides in guinea-pig bladder contractility.

作者信息

Longhurst P A, Briscoe J A, Rosenberg D J, Leggett R E

机构信息

Division of Urology, University of Pennsylvania Medical Center, Philadelphia 19104, USA.

出版信息

Br J Pharmacol. 1997 Aug;121(8):1665-72. doi: 10.1038/sj.bjp.0701328.

Abstract
  1. The effects of phosphodiesterase (PDE) inhibition and forskolin pretreatment on the contractile responses of guinea-pig urinary bladder strips to electrical field stimulation, carbachol, ATP and KCl were studied. 2. Inhibition of cyclic AMP-specific PDE4 isozymes by rolipram significantly reduced the contractile response of bladder strips to field stimulation. Rolipram also suppressed the contractile response to low concentrations of carbachol, but potentiated the response to high concentrations. The contractile response to ATP was significantly reduced by rolipram treatment, but that to KCl was unaltered. 3. Inhibition of cyclic GMP-specific PDE5 isozymes by zaprinast had no effects on the contractile response of bladder strips to field stimulation, ATP or KCl. Zaprinast suppressed the contractile responses to 1 microM carbachol and potentiated the response to high concentrations. 4. Contractile responses to field stimulation and to carbachol after pretreatment with the adenylyl cyclase activator, forskolin, were qualitatively similar to those caused by rolipram treatment. beta-Adrenoceptor blockade with propranolol partially reversed the inhibitory effects of rolipram on the response to field stimulation. 5. Rolipram significantly reduced the contractile response of bladder strips from sensitized guinea-pigs to ovalbumin challenge, but zaprinast was ineffective. PDE inhibition had similar effects on the responsiveness of control and of sensitized guinea-pig bladder strips to field stimulation, carbachol, ATP and KCl. 6. The data suggest that the contractile response of guinea-pig bladder strips can be modified by increases in cyclic AMP levels.
摘要
  1. 研究了磷酸二酯酶(PDE)抑制和福斯高林预处理对豚鼠膀胱条对电场刺激、卡巴胆碱、ATP和氯化钾收缩反应的影响。2. 咯利普兰对环磷酸腺苷特异性PDE4同工酶的抑制显著降低了膀胱条对电场刺激的收缩反应。咯利普兰还抑制了对低浓度卡巴胆碱的收缩反应,但增强了对高浓度卡巴胆碱的反应。咯利普兰处理显著降低了对ATP的收缩反应,但对氯化钾的收缩反应未改变。3. 扎普司特对环磷酸鸟苷特异性PDE5同工酶的抑制对膀胱条对电场刺激、ATP或氯化钾的收缩反应无影响。扎普司特抑制了对1微摩尔卡巴胆碱的收缩反应,并增强了对高浓度卡巴胆碱的反应。4. 用腺苷酸环化酶激活剂福斯高林预处理后,对电场刺激和卡巴胆碱的收缩反应在质量上与咯利普兰处理引起的反应相似。用普萘洛尔进行β肾上腺素能受体阻断部分逆转了咯利普兰对电场刺激反应的抑制作用。5. 咯利普兰显著降低了致敏豚鼠膀胱条对卵清蛋白攻击的收缩反应,但扎普司特无效。PDE抑制对对照和致敏豚鼠膀胱条对电场刺激、卡巴胆碱、ATP和氯化钾的反应性有类似影响。6. 数据表明,豚鼠膀胱条的收缩反应可通过环磷酸腺苷水平的升高而改变。

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