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由血管紧张素转换酶和糜酶构成的组织血管紧张素II生成系统。

Tissue angiotensin II generating system by angiotensin-converting enzyme and chymase.

作者信息

Miyazaki Mizuo, Takai Shinji

机构信息

Department of Pharmacology, Osaka Medical College, Japan.

出版信息

J Pharmacol Sci. 2006;100(5):391-7. doi: 10.1254/jphs.cpj06008x.

Abstract

It had been believed that angiotensin II (Ang II) was produced by the renin-angiotensin system (RAS), which was established in the 1950's. After a while, people realized that the multiple functions of Ang II could not be explained by the conventional RAS. We have tried to determine the existence of the tissue Ang II generating system. At first, we found that vascular angiotensin-converting enzyme (ACE) was increased to generate local Ang II in the vessels of hypertension and was enhanced in lipid-loaded atherosclerosis, to respond to ACE inhibitor or Ang II antagonist (ARB). In both cases, Ang II production in vessels was independent from the systemic RAS that was estimated by the plasma renin activity. On the way to clarifying the roles of the vascular ACE, we noticed that vascular Ang II production was not completely suppressed by ACE inhibitor alone. This evidence led us to discover different types of chymase as a new Ang II producing enzyme. Now, we have obtained a strategy to distinguish the Ang II one by one, that is, circulating RAS derived, tissue ACE derived, and chymase derived. It is essential to understand not only the intracellular mechanisms of Ang II but also the process of Ang II productions in each disease to show accurate indications of the effectiveness of ACE inhibitor, ARB, and chymase inhibitor.

摘要

人们曾认为血管紧张素II(Ang II)是由20世纪50年代建立的肾素-血管紧张素系统(RAS)产生的。一段时间后,人们意识到传统的RAS无法解释Ang II的多种功能。我们试图确定组织中Ang II生成系统的存在。起初,我们发现血管紧张素转换酶(ACE)在高血压血管中增加以产生局部Ang II,在脂质负荷的动脉粥样硬化中增强,以响应ACE抑制剂或Ang II拮抗剂(ARB)。在这两种情况下,血管中Ang II的产生都独立于通过血浆肾素活性估计的全身RAS。在阐明血管ACE作用的过程中,我们注意到仅用ACE抑制剂并不能完全抑制血管Ang II的产生。这一证据促使我们发现不同类型的糜酶作为一种新的Ang II产生酶。现在,我们已经获得了一种逐个区分Ang II的策略,即循环RAS衍生的、组织ACE衍生的和糜酶衍生的。不仅要了解Ang II的细胞内机制,还要了解每种疾病中Ang II的产生过程,以准确显示ACE抑制剂、ARB和糜酶抑制剂的有效性指征。

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