Ang-(1-7) and ET-1 Interplay Through Mas and ET_B Receptor Interaction Defines a Novel Vasoprotective Mechanism.

IF 6.9 1区医学 Q1 PERIPHERAL VASCULAR DISEASE

Hypertension Pub Date : 2025-02-01 Epub Date: 2024-12-05 DOI:10.1161/HYPERTENSIONAHA.124.22693

Augusto C Montezano, Jithin Kuriakose, Katie Y Hood, Yuan Yan Sin, Livia L Camargo, Yoon Namkung, Carlos H Castro, Robson A Santos, Rheure Alves-Lopes, Gonzalo Tejeda, Patricia Passaglia, Sehrish Basheer, Emily Gallen, Jane E Findlay, Fazli R Awan, Stéphane A Laporte, Margaret R MacLean, George S Baillie, Rhian M Touyz

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Abstract

Background: Ang-(1-7) (angiotensin (1-7)) via MasR (Mas receptor) opposes vaso-injurious actions of Ang II (angiotensin II) as shown in models of pulmonary hypertension. The underlying mechanisms remain unclear. We hypothesized cross talk between Ang-(1-7) and the protective arm of the ET-1 (endothelin-1) system involving MasR and ET_BR (endothelin receptor type B).

Methods: To address this, we studied multiple models: in vivo, in a mouse model of ET-1-associated vascular injury (hypoxia-induced pulmonary hypertension); ex vivo, in isolated mouse arteries; and in vitro, in human endothelial cells.

Results: Pulmonary hypertension mice exhibited pulmonary vascular remodeling, endothelial dysfunction, and ET-1-induced hypercontractility. Ang-(1-7) treatment (14 days) ameliorated these effects and increased the expression of vascular ET_BR. In human endothelial cells, Ang-(1-7)-induced activation of eNOS (endothelial NO synthase)/NO was attenuated by A779 (MasR antagonist) and BQ788 (ET_BR antagonist). A779 inhibited ET-1-induced signaling. Coimmunoprecipitation and peptide array experiments demonstrated the interaction between MasR and ET_BR. Binding sites for ET_BR were mapped to MasR (amino acids 290-314). Binding sites for MasR on ET_BR were identified (amino acids 176-200). Peptides that disrupt MasR:ET_BR prevented Ang-(1-7) and ET-1 signaling. Using high-throughput screening, we identified compounds that enhance MasR:ET_BR interaction, which we termed enhancers. Enhancers increased Ang-(1-7)-induced eNOS activity, NO production, and Ang-(1-7)-mediated vasorelaxation, and reduced contractile responses.

Conclusions: We identify cross talk between Ang-(1-7) and ET-1 through MasR:ET_BR interaction as a novel network that is vasoprotective. Promoting coactivity between these systems amplifies Ang-(1-7) signaling, increases ET-1/ET_BR-mediated vascular actions, and attenuates the injurious effects of ET-1. Enhancing Ang-(1-7)/MasR:ET-1/ET_BR signaling may have therapeutic potential in conditions associated with vascular damage.

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Ang-(1-7)和ET-1通过Mas和ETB受体相互作用定义了一种新的血管保护机制。

背景：在肺动脉高压模型中显示，Ang-(1-7)（血管紧张素（1-7））通过MasR （Mas受体）对抗Ang II（血管紧张素II）的血管损伤作用。其潜在机制尚不清楚。我们假设Ang-(1-7)与ET-1（内皮素-1）系统的保护臂之间存在串扰，包括MasR和ETBR（内皮素受体B型）。方法/结果：为了解决这一问题，我们研究了多种模型：在体内，在ET-1相关血管损伤（缺氧诱导的肺动脉高压）的小鼠模型中；离体小鼠动脉；在体外，在人类内皮细胞中。肺动脉高压小鼠表现出肺血管重构、内皮功能障碍和et -1诱导的过度收缩。Ang-(1-7)治疗（14天）改善了这些效果，并增加了血管ETBR的表达。在人内皮细胞中，Ang-(1-7)诱导的eNOS（内皮NO合成酶）/NO的激活被A779 （MasR拮抗剂）和BQ788 （ETBR拮抗剂）减弱。A779抑制et -1诱导的信号传导。共免疫沉淀和肽阵列实验证实了MasR与ETBR之间的相互作用。ETBR的结合位点被定位到MasR（氨基酸290-314）。确定了ETBR上MasR的结合位点（氨基酸176 ~ 200）。破坏MasR:ETBR的肽可阻止Ang-(1-7)和ET-1信号传导。通过高通量筛选，我们确定了增强MasR:ETBR相互作用的化合物，我们称之为增强剂。增强剂增加Ang-(1-7)诱导的eNOS活性、NO生成和Ang-(1-7)介导的血管松弛，并减少收缩反应。结论：我们通过MasR:ETBR相互作用确定Ang-(1-7)和ET-1之间的串扰是一个具有血管保护作用的新网络。促进这些系统之间的协同作用可以放大Ang-(1-7)信号，增加ET-1/ etbr介导的血管活动，并减弱ET-1的有害作用。增强Ang-(1-7)/MasR:ET-1/ETBR信号可能对血管损伤相关疾病具有治疗潜力。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Hypertension 医学-外周血管病

CiteScore

15.90

自引率

4.80%

发文量

1006

审稿时长

1 months

期刊介绍： Hypertension presents top-tier articles on high blood pressure in each monthly release. These articles delve into basic science, clinical treatment, and prevention of hypertension and associated cardiovascular, metabolic, and renal conditions. Renowned for their lasting significance, these papers contribute to advancing our understanding and management of hypertension-related issues.