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啮齿动物和人类中血管紧张素 II 形成途径的演变故事。

An evolving story of angiotensin-II-forming pathways in rodents and humans.

机构信息

§Birmingham Veterans Affair Medical Center, University of Alabama Medical Center, Alabama, AL 35294, U.S.A.

出版信息

Clin Sci (Lond). 2014 Apr;126(7):461-9. doi: 10.1042/CS20130400.

Abstract

Lessons learned from the characterization of the biological roles of Ang-(1-7) [angiotensin-(1-7)] in opposing the vasoconstrictor, proliferative and prothrombotic actions of AngII (angiotensin II) created an underpinning for a more comprehensive exploration of the multiple pathways by which the RAS (renin-angiotensin system) of blood and tissues regulates homoeostasis and its altered state in disease processes. The present review summarizes the progress that has been made in the novel exploration of intermediate shorter forms of angiotensinogen through the characterization of the expression and functions of the dodecapeptide Ang-(1-12) [angiotensin-(1-12)] in the cardiac production of AngII. The studies reveal significant differences in humans compared with rodents regarding the enzymatic pathway by which Ang-(1-12) undergoes metabolism. Highlights of the research include the demonstration of chymase-directed formation of AngII from Ang-(1-12) in human left atrial myocytes and left ventricular tissue, the presence of robust expression of Ang-(1-12) and chymase in the atrial appendage of subjects with resistant atrial fibrillation, and the preliminary observation of significantly higher Ang-(1-12) expression in human left atrial appendages.

摘要

从 Ang-(1-7)[血管紧张素-(1-7)]在拮抗 AngII(血管紧张素 II)的血管收缩、增殖和促血栓作用的生物学作用的特征中吸取的经验教训,为更全面地探索血液和组织中的 RAS(肾素-血管紧张素系统)调节体内平衡及其在疾病过程中改变状态的多种途径奠定了基础。本综述总结了通过对心脏产生的 AngII 中十二肽 Ang-(1-12)[血管紧张素-(1-12)]的表达和功能的特征研究,在探索血管紧张素原中间较短形式方面取得的进展。与啮齿动物相比,这些研究在 Ang-(1-12) 代谢的酶促途径方面显示出显著差异。研究的重点包括证明糜酶可将 Ang-(1-12) 定向转化为 AngII,在人类左心房心肌细胞和左心室组织中,Ang-(1-12) 和糜酶的表达水平较高,在对心房颤动有抗性的患者的心房附肢中存在丰富的 Ang-(1-12) 和糜酶表达,以及在人类左心房附肢中观察到 Ang-(1-12) 表达显著升高的初步观察。

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