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Role of the vasodilator peptide angiotensin-(1–7) in cardiovascular drug therapy

机译:血管扩张肽血管紧张素-(1-7)在心血管药物治疗中的作用

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摘要

The renin-angiotensin-system (RAS) is a cascade of enzymatic reactions resulting ultimately in the formation of angiotensin II. Recent research has expanded the knowledge about the RAS by adding new components to the pathways: angiotensin-(1–5) [Ang-1–5], angiotensin-(1–7) [Ang-(1–7)], angiotensin-(1–9) [Ang-(1–9)], an ACE homologous enzyme, ACE2, and the G-protein-coupled receptor mas as a molecular receptor for Ang-(1–7). Although previous studies provided some conflicting evidence about the relevance of Ang-(1–7) in the regulation of vascular and renal function, data now demonstrate that Ang-(1–7) contributes to the cardiovascular effects of ACE-inhibitors (ACE-I) and AT1-receptor-blockers (ARBs) both in experimental conditions and in humans. This review summarizes and critically discusses the currently available experimental and clinical study evidence for the role of Ang-(1–7) as a vasodilator and anti-trophic peptide in cardiovascular drug therapy. In addition, the potential therapeutic impact of currently available RAS blocking agents (ACE-I and ARBs) and new agents still under development (renin-inhibitors) on the RAS-effector peptides is highlighted.
机译:肾素-血管紧张素系统(RAS)是一连串的酶促反应,最终导致血管紧张素II的形成。最近的研究通过向途径添加新的成分来扩展了对RAS的了解:血管紧张素(1-5)[Ang-1-5],血管紧张素(1-7)[Ang-(1-7)],血管紧张素-(1–9)[Ang-(1–9)],一种ACE同源酶ACE2和G蛋白偶联受体mas作为Ang-(1–7)的分子受体。尽管先前的研究提供了一些有关Ang-(1-7)在调节血管和肾功能中的相关性的相互矛盾的证据,但现在的数据表明Ang-(1-7)有助于ACE抑制剂(ACE- I)和AT1受体阻滞剂(ARB)在实验条件下和在人类中均如此。这篇综述总结并批判性地讨论了Ang-(1-7)作为血管扩张药和抗营养肽在心血管药物治疗中的作用的当前可用的实验和临床研究证据。另外,突出了当前可用的RAS封闭剂(ACE-1和ARB)和仍在开发中的新试剂(肾素抑制剂)对RAS效应子肽的潜在治疗作用。

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