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Direct role for smooth muscle cell mineralocorticoid receptors in vascular remodeling: Novel mechanisms and clinical implications

机译:平滑肌细胞盐皮质激素受体在血管重塑中的直接作用:新机制和临床意义

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摘要

The mineralocorticoid receptor (MR) is a key regulator of blood pressure. MR antagonist drugs are used to treat hypertension and heart failure, resulting in decreased mortality by mechanisms that are not completely understood. In addition to the kidney, MR is also expressed in the smooth muscle cells (SMCs) of the vasculature, where it is activated by the hormone aldosterone and affects the expression of genes involved in vascular function at the cellular and systemic levels. Following vascular injury due to mechanical or physiological stresses, vessels undergo remodeling resulting in SMC hypertrophy, migration, and proliferation, as well as vessel fibrosis. Exuberant vascular remodeling is associated with poor outcomes in cardiovascular patients. This review compiles recent findings on the specific role of SMC-MR in the vascular remodeling process. The development and characterization of a SMC-specific MR-knockout mouse has demonstrated a direct role for SMC-MR in vascular remodeling. Additionally, several novel mechanisms contributing to SMC-MR-mediated vascular remodeling have been identified and are reviewed here, including Rho-kinase signaling, placental growth factor signaling through vascular endothelial growth factor type 1 receptor, and galectin signaling.
机译:盐皮质激素受体(MR)是血压的关键调节剂。 MR拮抗剂药物用于治疗高血压和心力衰竭,其机制尚不完全清楚,导致死亡率降低。除肾脏外,MR还表达于脉管系统的平滑肌细胞(SMC)中,并在此被激素醛固酮激活,并在细胞和全身水平上影响参与血管功能的基因的表达。在由于机械或生理压力引起的血管损伤后,血管进行重塑,导致SMC肥大,迁移和增殖以及血管纤维化。旺盛的血管重塑与心血管患者预后不良有关。这篇综述汇编了有关SMC-MR在血管重塑过程中特定作用的最新发现。 SMC特定的MR基因敲除小鼠的发展和特征已证明SMC-MR在血管重塑中的直接作用。此外,已鉴定并综述了促成SMC-MR介导的血管重塑的几种新颖机制,包括Rho激酶信号传导,通过血管内皮生长因子1型受体的胎盘生长因子信号传导和半乳凝素信号传导。

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