miR-145 Alleviates Smooth Muscle Cell Phenotype Transition via ADAM17-Mediated ACE2 Shedding.

IF 1.9 4区 医学 Q3 PERIPHERAL VASCULAR DISEASE
Juan Wen, Baiyi Tang, Lan Guo, Wei Chen, Xiaohong Tang
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Abstract

It has been shown that miR-145 is involved in the differentiation of vascular smooth muscle cells (VSMCs) and may regulate vascular remodeling. However, the molecular mechanisms behind these pathological processes in hypertension are not fully elucidated. The present study was to examine whether miR-145 modulates phenotypic transformation of VSMCs under normal state and synthetic state and to explore the possible role of ADAM17-mediated ACE2 shedding and ACE2-Ang-(1-7)-Mas receptor axis. Wistar rats were fed with high-sucrose/high-fat diet for 30 weeks to establish a metabolic hypertension animal model. VSMCs were cultured and treated with Ang II with or without miR-145 mimics or miR-145 inhibitor. Results showed the expression of contractile markers α-SMA and SM22α, miR-145, ACE2, and Mas receptor reduced in the thoracic aorta of metabolic hypertensive rats (MHRs), while that of synthetic marker OPN increased as compared to the control group. In in vitro study, miR-145 inhibitor inhibited the expression of α-SMA, SM22α, ACE2, Mas receptor, and the Ang-(1-7) excretion and induced the expression of synthetic markers OPN, EREG, and MMP2. However, miR-145 mimic produced opposite effects on the VSMCs. In addition, in the synthetic VSMC induced by Ang II, miR-145 inhibitor partially reversed the induced expression of OPN, EREG, and MMP2 by Ang II, while further decreasing the expression of α-SMA and SM22α and ACE2-Ang-(1-7)-Mas receptor. Cotreatment with ADAM17 siRNA partially reversed the inducible effect of miR-145 inhibitor on the EREG and MMP2, induced Ang-(1-7) excretion, and upregulated ACE2 and Mas receptor expression. In conclusion, miR-145 alleviates phenotype transition from contractile to synthetic type via ADAM17-mediated ACE2 shedding in VSMCs and retains the activation of ACE2-Ang-(1-7)-Mas axis, which may benefit the vascular structural remodeling in the metabolic hypertension.

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miR-145通过adam17介导的ACE2脱落缓解平滑肌细胞表型转变
研究表明,miR-145参与血管平滑肌细胞(VSMCs)的分化,并可能调节血管重塑。然而,这些病理过程背后的分子机制在高血压尚未完全阐明。本研究旨在检测miR-145是否在正常状态和合成状态下调节VSMCs的表型转化,并探讨adam17介导的ACE2脱落和ACE2- ang -(1-7)- mas受体轴的可能作用。采用高糖高脂饲料喂养Wistar大鼠30周,建立代谢性高血压动物模型。培养VSMCs,并用含或不含miR-145模拟物或miR-145抑制剂的Ang II处理。结果显示,代谢性高血压大鼠胸主动脉收缩标志物α-SMA、SM22α、miR-145、ACE2、Mas受体的表达与对照组相比降低,合成标志物OPN的表达与对照组相比升高。在体外研究中,miR-145抑制剂抑制α-SMA、SM22α、ACE2、Mas受体的表达和Ang-(1-7)的排泄,诱导合成标记物OPN、EREG、MMP2的表达。然而,miR-145模拟物对vsmc产生相反的作用。此外,在Ang II诱导的合成VSMC中,miR-145抑制剂部分逆转了Ang II诱导的OPN、EREG和MMP2的表达,同时进一步降低α-SMA、SM22α和ACE2-Ang-(1-7)- mas受体的表达。与ADAM17 siRNA共处理部分逆转了miR-145抑制剂对EREG和MMP2的诱导作用,诱导Ang-(1-7)排泄,上调ACE2和Mas受体表达。综上所述,miR-145通过adam17介导的VSMCs中ACE2的脱落,减轻了从收缩型到合成型的表型转变,并保持了ACE2- ang -(1-7)- mas轴的激活,这可能有利于代偿性高血压的血管结构重塑。
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来源期刊
International Journal of Hypertension
International Journal of Hypertension Medicine-Internal Medicine
CiteScore
4.00
自引率
5.30%
发文量
45
期刊介绍: International Journal of Hypertension is a peer-reviewed, Open Access journal that provides a forum for clinicians and basic scientists interested in blood pressure regulation and pathophysiology, as well as treatment and prevention of hypertension. The journal publishes original research articles, review articles, and clinical studies on the etiology and risk factors of hypertension, with a special focus on vascular biology, epidemiology, pediatric hypertension, and hypertensive nephropathy.
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