Angiotensin II Induces Vascular Endothelial Dysfunction by Promoting Lipid Peroxidation-Mediated Ferroptosis via CD36.

IF 4.8 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Biomolecules Pub Date : 2024-11-17 DOI:10.3390/biom14111456
Qian Zhou, Ying Zhang, Wei Shi, Lu Lu, Jianglan Wei, Jinhan Wang, Hu Zhang, Yuepu Pu, Lihong Yin
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引用次数: 0

Abstract

Angiotensin II (Ang II) is an effective vasoconstriction peptide, a major effector molecule of the renin-angiotensin-aldosterone system (RAAS) and one of the important causes of endothelial dysfunction. Ferroptosis is considered to be involved in the occurrence and development of cardiovascular diseases. This study is dedicated to exploring the role and mechanism of Ang II-induced ferroptosis in HUVECs and to finding molecular targets for vascular endothelial injury and dysfunction during the progression of hypertension. In this study, we found that with the increase in exposure concentration, the intracellular ROS content and apoptosis rate increased significantly, the NO release decreased significantly in the medium- and high-concentration groups and the ET-1 content in the high-concentration group increased significantly. The expression of ZO-1 protein was significantly decreased in the high-concentration group. The expression of p-eNOS, VE-cadherin and Occludin protein showed a dose-dependent downward trend, while the ICAM-1 protein showed an upward trend. Ang II caused lipid metabolism disorders in HUVECs, and the PL-PUFAs associated with ferroptosis were significantly increased. In addition, Ang II promoted a significant increase in intracellular free Fe2+ content and MDA and a significant decrease in GSH content. Furthermore, the expression of GPX4, SLC7A11 and SLC3A2 was down-regulated, the expression of ACSL4, LPCAT3 and ALOX15 was up-regulated, and the ratio of p-cPLA2/cPLA2 was increased. After the intervention of ferroptosis inhibitor Fer-1, the injury and dysfunction of HUVECs induced by Ang II were significantly rescued. Immunofluorescence results showed that the expression of CD36 showed a significant increasing trend and was localized in the cytoplasm. Over-expression of CD36 promoted Ang II-induced ferroptosis and endothelial dysfunction. In conclusion, Ang II induces the injury of HUVECs, decreases vascular diastole and endothelial barrier-related molecules, and increases vascular constriction and adhesion-related molecules, which may be related to CD36 and its mediated lipid peroxidation and ferroptosis signals.

血管紧张素 II 通过 CD36 促进脂质过氧化介导的铁氧化诱导血管内皮功能障碍
血管紧张素 II(Ang II)是一种有效的血管收缩肽,是肾素-血管紧张素-醛固酮系统(RAAS)的主要效应分子,也是导致内皮功能障碍的重要原因之一。铁蛋白沉积被认为与心血管疾病的发生和发展有关。本研究致力于探索 Ang II 诱导的 HUVECs 铁蛋白沉积的作用和机制,并寻找高血压进展过程中血管内皮损伤和功能障碍的分子靶点。本研究发现,随着暴露浓度的增加,细胞内 ROS 含量和细胞凋亡率显著增加,中、高浓度组 NO 释放量显著减少,高浓度组 ET-1 含量显著增加。高浓度组 ZO-1 蛋白表达明显下降。p-eNOS、VE-cadherin和Occludin蛋白的表达呈剂量依赖性下降趋势,而ICAM-1蛋白的表达呈上升趋势。Ang II导致HUVECs脂质代谢紊乱,与铁变态反应相关的PL-PUFAs显著增加。此外,Ang II 还促进细胞内游离 Fe2+ 含量和 MDA 含量显著增加,GSH 含量显著减少。此外,GPX4、SLC7A11 和 SLC3A2 的表达下调,ACSL4、LPCAT3 和 ALOX15 的表达上调,p-cPLA2/cPLA2 的比值升高。在铁蛋白沉积抑制剂 Fer-1 的干预下,Ang II 诱导的 HUVECs 损伤和功能障碍得到明显缓解。免疫荧光结果显示,CD36的表达呈显著上升趋势,并定位于细胞质中。CD36 的过度表达促进了 Ang II 诱导的铁沉积和内皮功能障碍。总之,Ang II诱导HUVECs损伤,减少血管舒张和内皮屏障相关分子,增加血管收缩和粘附相关分子,这可能与CD36及其介导的脂质过氧化和铁蛋白沉积信号有关。
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
Biomolecules
Biomolecules Biochemistry, Genetics and Molecular Biology-Molecular Biology
CiteScore
9.40
自引率
3.60%
发文量
1640
审稿时长
18.28 days
期刊介绍: Biomolecules (ISSN 2218-273X) is an international, peer-reviewed open access journal focusing on biogenic substances and their biological functions, structures, interactions with other molecules, and their microenvironment as well as biological systems. Biomolecules publishes reviews, regular research papers and short communications.  Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced.
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