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作为支气管扩张剂和平滑肌松弛剂的茶碱和选择性磷酸二酯酶抑制剂。

Theophylline and selective PDE inhibitors as bronchodilators and smooth muscle relaxants.

作者信息

Rabe K F, Magnussen H, Dent G

机构信息

Krankenhaus Grosshansdorf, Zentrum für Pneumologie und Thoraxchirurgie, LVA, Hamburg, Germany.

出版信息

Eur Respir J. 1995 Apr;8(4):637-42.

PMID:7664866
Abstract

In addition to its emerging immunodulatory properties, theophylline is a bronchodilator and also decreases mean pulmonary arterial pressure in vivo. The mechanism of action of this drug remains controversial; adenosine antagonism, phosphodiesterase (PDE) inhibition and other actions have been advanced to explain its effectiveness in asthma. Cyclic adenosine monophosphate (AMP) and cyclic guanosine monophosphate (GMP) are involved in the regulation of smooth muscle tone, and the breakdown of these nucleotides is catalysed by multiple PDE isoenzymes. The PDE isoenzymes present in human bronchus and pulmonary artery have been identified, and the pharmacological actions of inhibitors of these enzymes have been investigated. Human bronchus and pulmonary arteries are relaxed by theophylline and by selective inhibitors of PDE III, while PDE IV inhibitors also relax precontracted bronchus and PDE V/I inhibitors relax pulmonary artery. There appears to be some synergy between inhibitors of PDE III and PDE IV in relaxing bronchus, and a pronounced synergy between PDE III and PDE V inhibitors in relaxing pulmonary artery. In neither tissue does 8-phenyltheophylline, a xanthine exhibiting adenosine antagonism but not PDE inhibition, cause any significant relaxation, implying that theophylline does not exert its actions through adenosine antagonism. The close correspondence of theophylline concentrations inhibiting bronchus or pulmonary artery PDE and those causing relaxation points towards PDE inhibition as the major mechanism of action of theophylline in smooth muscle relaxation.

摘要

除了其新出现的免疫调节特性外,茶碱还是一种支气管扩张剂,并且在体内可降低平均肺动脉压。该药物的作用机制仍存在争议;腺苷拮抗、磷酸二酯酶(PDE)抑制及其他作用已被提出以解释其在哮喘中的有效性。环磷酸腺苷(AMP)和环磷酸鸟苷(GMP)参与平滑肌张力的调节,这些核苷酸的分解由多种PDE同工酶催化。已鉴定出存在于人类支气管和肺动脉中的PDE同工酶,并对这些酶抑制剂的药理作用进行了研究。茶碱和PDE III选择性抑制剂可使人类支气管和肺动脉舒张,而PDE IV抑制剂也可使预收缩的支气管舒张,PDE V/I抑制剂可使肺动脉舒张。在舒张支气管方面,PDE III和PDE IV抑制剂之间似乎存在一些协同作用,而在舒张肺动脉方面,PDE III和PDE V抑制剂之间存在明显的协同作用。在这两种组织中,8-苯基茶碱(一种具有腺苷拮抗作用但无PDE抑制作用的黄嘌呤)均不会引起任何明显的舒张,这意味着茶碱并非通过腺苷拮抗作用发挥其作用。抑制支气管或肺动脉PDE的茶碱浓度与引起舒张的浓度密切相关,这表明PDE抑制是茶碱在平滑肌舒张中发挥作用的主要机制。

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Eur Respir J. 1995 Apr;8(4):637-42.
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