miR-432-5p通过降解Keap1激活Nrf2/SLC7A11轴抑制缺氧/再氧诱导的心肌细胞脱铁。

IF 2.6 4区 医学 Q3 CELL BIOLOGY Analytical Cellular Pathology Pub Date : 2023-10-03 eCollection Date: 2023-01-01 DOI:10.1155/2023/1293200
Wei Geng, Shaohua Yan, Xinyue Li, Qiumei Liu, Xuefei Zhang, Xinshun Gu, Xiang Tian, Yunfa Jiang
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引用次数: 0

摘要

缺血后早期心肌再灌注导致心肌缺血再灌注(I/R)损伤,并涉及脱铁性贫血。缺血激活一系列氧化应激基因及其下游调控基因的表达,包括脱铁相关基因,如核因子E2相关因子2(Nrf2)、谷胱甘肽过氧化物酶4(GPX4)和SLC7A11。本研究采用大鼠原代心肌细胞和I/R来评价体内外Nrf2-SLC7A11/血红素加氧酶-1(HO-1)的脱铁作用和变化。在线分析工具用于预测miR-432-5p的可能靶向Kelch样ECH相关蛋白1(Keap1)。构建miR-432-5p质粒的模拟物以验证miR-432-5p对脱铁性贫血的影响。我们发现心肌细胞缺氧/复氧(H/R)和大鼠I/R可诱导心肌细胞脂质过氧化和脱铁性贫血。Nrf2-SLC7A11/HO-1通路的激活保护心肌细胞免于脱铁性贫血。miR-432-5p的下调已在H/R心肌细胞(体外)和心肌梗死大鼠的心肌细胞(体内)中得到证实。miR-432-5p的上调通过降低Nrf2、Keap1的结合蛋白来抑制由RAS选择性致死3(RSL3)诱导的心肌细胞脱铁性贫血,这一点已通过生物信息学和突变分析得到证实。敲低Nrf2减弱miR-432-5p对H/R心肌细胞的保护作用。静脉递送miR-432-5p脂质体载体显著改善I/R动物模型中的心肌细胞损伤。总之,miR-432-5p通过降解Keap1来激活Nrf2/SLC7A11轴,从而抑制H/R诱导的心肌细胞脱铁性贫血,是临床心肌梗死治疗的潜在药物靶点。
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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miR-432-5p Inhibits the Ferroptosis in Cardiomyocytes Induced by Hypoxia/Reoxygenation via Activating Nrf2/SLC7A11 Axis by Degrading Keap1.

Early reperfusion into the myocardium after ischemia causes myocardial ischemia-reperfusion (I/R) injury and ferroptosis was involved. Ischemia activates the expression of a series of oxidative stress genes and their downstream regulatory genes, including ferroptosis-related genes such as nuclear factor E2-related factor 2 (Nrf2), glutathione peroxidase 4 (GPX4), and SLC7A11. This study adopted primary cardiomyocytes and I/R in rats to evaluate the ferroptosis and changing of Nrf2-SLC7A11/heme oxygenase-1 (HO-1) in vitro and in vivo. Online analysis tools were used to predict the possible target Kelch-like ECH-associated protein 1 (Keap1) of miR-432-5p. The mimic of miR-432-5p plasmid was constructed to verify the effect of miR-432-5p on ferroptosis. We found that hypoxia/reoxygenation (H/R) in cardiomyocytes and I/R in rats induced lipid peroxidation and ferroptosis in cardiomyocytes. The activation of the Nrf2-SLC7A11/HO-1 pathway protects cardiomyocytes from ferroptosis. Downregulation of miR-432-5p has been confirmed in H/R cardiomyocytes (in vitro) and cardiomyocytes in myocardial infarction rats (in vivo). Upregulation of miR-432-5p inhibited ferroptosis of cardiomyocytes induced by RAS-selective lethal 3 (RSL3), an inhibitor of GPX4 and ferroptosis inducer through decreasing the binding protein of Nrf2, Keap1, which was confirmed by bioinformatics and mutation assay. Knockdown Nrf2 attenuates the protection effect of miR-432-5p on H/R cardiomyocytes. Intravenous delivery of liposome carriers of miR-432-5p remarkably ameliorated cardiomyocyte impairment in the I/R animal model. In conclusion, miR-432-5p inhibits the ferroptosis in cardiomyocytes induced by H/R by activating Nrf2/SLC7A11 axis by degrading Keap1 and is a potential drug target for clinical myocardial infarction treatment.

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来源期刊
Analytical Cellular Pathology
Analytical Cellular Pathology ONCOLOGY-CELL BIOLOGY
CiteScore
4.90
自引率
3.10%
发文量
70
审稿时长
16 weeks
期刊介绍: Analytical Cellular Pathology is a peer-reviewed, Open Access journal that provides a forum for scientists, medical practitioners and pathologists working in the area of cellular pathology. The journal publishes original research articles, review articles, and clinical studies related to cytology, carcinogenesis, cell receptors, biomarkers, diagnostic pathology, immunopathology, and hematology.
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