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血管紧张素转换酶抑制剂对组织抑制作用的比较研究。

Comparative studies of tissue inhibition by angiotensin converting enzyme inhibitors.

作者信息

Johnston C I, Fabris B, Yamada H, Mendelsohn F A, Cubela R, Sivell D, Jackson B

机构信息

Department of Medicine, Melbourne University, Austin hospital, Heidelberg, Victoria, Australia.

出版信息

J Hypertens Suppl. 1989 Sep;7(5):S11-6.

PMID:2553899
Abstract

There is increasing evidence that inhibition of tissue angiotensin converting enzyme (ACE) is important for the pharmacokinetics and pharmacodynamic effects of ACE inhibitors. Radioligand inhibitor binding methods using 125I-351A and either tissue homogenates or in vitro autoradiography have allowed in vitro and ex vivo quantitation of tissue ACE inhibition by a variety of ACE inhibitors. The rank order of potency against plasma as well as lung, kidney, and cardiac homogenates was quinaprilat = benazeprilat greater than perindoprilat greater than lisinopril greater than enalaprilat greater than fosinoprilat. The highest concentration of ACE in the heart was found in the cardiac valves followed by the right and left atria, then the right and left ventricles. Ex vivo studies showed that after oral administration of quinapril, ACE was inhibited dose-dependently in the lung, kidney, aorta and heart for more than 24h. Tissue bioavailability of the inhibitor is also an important determinant of tissue ACE inhibition. Perindopril crossed the blood-brain barrier and inhibited brain ACE at high doses, but after equivalent doses of quinapril no brain ACE inhibition could be demonstrated. These results suggest that it may be possible to design ACE inhibitors to have specific effects on ACE in different tissues.

摘要

越来越多的证据表明,抑制组织血管紧张素转换酶(ACE)对ACE抑制剂的药代动力学和药效学作用至关重要。使用125I-351A以及组织匀浆或体外放射自显影的放射性配体抑制剂结合方法,已能够对多种ACE抑制剂在体外和体内对组织ACE的抑制作用进行定量分析。对血浆以及肺、肾和心脏匀浆的抑制效力排序为:喹那普利拉 = 贝那普利拉>培哚普利拉>赖诺普利>依那普利拉>福辛普利拉。心脏中ACE浓度最高的部位是心脏瓣膜,其次是右心房和左心房,然后是右心室和左心室。体内研究表明,口服喹那普利后,肺、肾、主动脉和心脏中的ACE被剂量依赖性抑制超过24小时。抑制剂的组织生物利用度也是组织ACE抑制的一个重要决定因素。培哚普利可穿过血脑屏障并在高剂量时抑制脑ACE,但给予等效剂量的喹那普利后,未显示出对脑ACE的抑制作用。这些结果表明,有可能设计出对不同组织中的ACE具有特定作用的ACE抑制剂。

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