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心血管系统及其他系统中的原肾素受体。

The prorenin receptor in the cardiovascular system and beyond.

机构信息

Department of Physiology, Tulane University School of Medicine , New Orleans, Louisiana.

Instituto de Química, Pontificia Universidad Católica de Valparaíso , Valparaíso , Chile.

出版信息

Am J Physiol Heart Circ Physiol. 2018 Feb 1;314(2):H139-H145. doi: 10.1152/ajpheart.00373.2017. Epub 2017 Nov 3.

Abstract

Since the prorenin receptor (PRR) was first reported, its physiological role in many cellular processes has been under intense scrutiny. The PRR is currently recognized as a multifunctional receptor with major roles as an accessory protein of the vacuolar-type H-ATPase and as an intermediary in the Wnt signaling pathway. As a member of the renin-angiotensin system (RAS), the PRR has demonstrated to be of relevance in cardiovascular diseases (CVD) because it can activate prorenin and enhance the enzymatic activity of renin, thus promoting angiotensin II formation. Indeed, there is an association between PRR gene polymorphisms and CVD. Independent of angiotensin II, the activation of the PRR further stimulates intracellular signals linked to fibrosis. Studies using tissues and cells from a variety of organs and systems have supported its roles in multiple functions, although some remain controversial. In the brain, the PRR appears to be involved in the central regulation of blood pressure via activation of RAS- and non-RAS-dependent mechanisms. In the heart, the PRR promotes atrial structural and electrical remodeling. Nonetheless, animals overexpressing the PRR do not exhibit cardiac injury. In the kidney, the PRR is involved in the development of ureteric bud branching, urine concentration, and regulation of blood pressure. There is great interest in the PRR contributions to T cell homeostasis and to the development of visceral and brown fat. In this mini-review, we discuss the evidence for the pathophysiological roles of the PRR with emphasis in CVD.

摘要

自从原肾素受体(PRR)首次被报道以来,其在许多细胞过程中的生理作用一直受到广泛关注。PRR 目前被认为是一种多功能受体,主要作为液泡型 H+-ATP 酶的辅助蛋白和 Wnt 信号通路的中介发挥作用。作为肾素-血管紧张素系统(RAS)的一员,PRR 已被证明与心血管疾病(CVD)有关,因为它可以激活原肾素并增强肾素的酶活性,从而促进血管紧张素 II 的形成。事实上,PRR 基因多态性与 CVD 之间存在关联。独立于血管紧张素 II,PRR 的激活进一步刺激与纤维化相关的细胞内信号。使用来自各种器官和系统的组织和细胞进行的研究支持了其在多种功能中的作用,尽管有些仍存在争议。在大脑中,PRR 似乎通过激活 RAS 和非 RAS 依赖的机制参与血压的中枢调节。在心脏中,PRR 促进心房结构和电重构。尽管如此,过表达 PRR 的动物并没有表现出心脏损伤。在肾脏中,PRR 参与输尿管芽分支、尿液浓缩和血压调节的发育。PRR 对 T 细胞稳态和内脏脂肪和棕色脂肪发育的贡献引起了极大的兴趣。在这篇小型综述中,我们讨论了 PRR 的病理生理作用的证据,重点是 CVD。

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