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肾素血管紧张素阻滞剂与心脏保护:从基础到临床试验。

Renin Angiotensin Blockers and Cardiac Protection: From Basis to Clinical Trials.

机构信息

Inserm U970, PARRC, Hôpital Lariboisière, Paris, France.

Hôpital St Joseph, Paris, France.

出版信息

Am J Hypertens. 2022 Apr 2;35(4):293-302. doi: 10.1093/ajh/hpab108.

Abstract

Despite a similar beneficial effect on blood pressure lowering observed with angiotensin-converting enzyme inhibitors (ACEIs) and angiotensin II type 1 receptor (AT1R) blocker (ARBs), several clinical trials and meta-analyses have reported higher cardiovascular mortality and lower protection against myocardial infarction with ARBs when compared with ACEIs. The European guidelines for the management of coronary syndromes and European guidelines on diabetes recommend using ARBs in patients who are intolerant to ACEIs. We reviewed the main pharmacological differences between ACEIs and ARBs, which could provide insights into the differences in the cardiac protection offered by these 2 drug classes. The effect of ACEIs on the tissue and plasma levels of bradykinin and on nitric oxide production and bioavailability is specific to the mechanism of action of ACEIs; it could account for the different effects of ACEIs and ARBs on endothelial function, atherogenesis, and fibrinolysis. Moreover, chronic blockade of AT1 receptors by ARBs induces a significant and permanent increase in plasma angiotensin II and an overstimulation of its still available receptors. In animal models, AT4 receptors have vasoconstrictive, proliferative, and inflammatory effects. Moreover, in models with kidney damage, atherosclerosis, and/or senescence, activation of AT2 receptors could have deleterious fibrotic, vasoconstrictive, and hypertrophic effects and seems prudent and reasonable to reserve the use of ARBs for patients who have presented intolerance to ACE inhibitors.

摘要

尽管血管紧张素转换酶抑制剂 (ACEIs) 和血管紧张素 II 型 1 型受体 (AT1R) 阻滞剂 (ARBs) 在降低血压方面观察到类似的有益效果,但几项临床试验和荟萃分析报告称,与 ACEIs 相比,ARBs 可降低心肌梗死的发生风险,但心血管死亡率更高。欧洲冠状动脉综合征管理指南和欧洲糖尿病指南建议在不能耐受 ACEIs 的患者中使用 ARBs。我们回顾了 ACEIs 和 ARBs 之间的主要药理学差异,这可以深入了解这两类药物在心脏保护方面的差异。ACEIs 对缓激肽的组织和血浆水平以及一氧化氮的产生和生物利用度的影响是 ACEIs 作用机制特异性的;这可能解释了 ACEIs 和 ARBs 对内皮功能、动脉粥样硬化和纤溶的不同影响。此外,ARBs 对 AT1 受体的慢性阻断会导致血浆血管紧张素 II 显著且永久性增加,并过度刺激其仍可用的受体。在动物模型中,AT4 受体具有血管收缩、增殖和炎症作用。此外,在肾损伤、动脉粥样硬化和/或衰老的模型中,AT2 受体的激活可能具有有害的纤维化、血管收缩和肥大作用,因此保留 ARBs 用于对 ACE 抑制剂不耐受的患者似乎是谨慎和合理的。

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