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首页> 外文期刊>Redox Biology >MicroRNA-140-5p aggravates doxorubicin-induced cardiotoxicity by promoting myocardial oxidative stress via targeting Nrf2 and Sirt2
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MicroRNA-140-5p aggravates doxorubicin-induced cardiotoxicity by promoting myocardial oxidative stress via targeting Nrf2 and Sirt2

机译:MicroRNA-140-5p通过靶向Nrf2和Sirt2促进心肌氧化应激,加剧了阿霉素诱导的心脏毒性

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Clinical application of doxorubicin (DOX), an anthracycline antibiotic with potent anti- tumor effects, is limited because of its cardiotoxicity. However, its pathogenesis is still not entirely understood. The aim of this paper was to explore the mechanisms and new drug targets to treat DOX-induced cardiotoxicity. The in vitro model on H9C2 cells and the in vivo models on rats and mice were developed. The results showed that DOX markedly decreased H9C2 cell viability, increased the levels of CK, LDH, caused histopathological and ECG changes in rats and mice, and triggered myocardial oxidative damage via adjusting the levels of intracellular ROS, MDA, SOD, GSH and GSH-Px. Total of 18 differentially expressed microRNAs in rat heart tissue caused by DOX were screened out using microRNA microarray assay, especially showing that miR-140-5p was significantly increased by DOX which was selected as the target miRNA. Double-luciferase reporter assay showed that miR-140-5p directly targeted Nrf2 and Sirt2, as a result of affecting the expression levels of HO-1, NQO1, Gst, GCLM, Keap1 and FOXO3a, and thereby increasing DOX-caused myocardial oxidative damage. In addition, the levels of intracellular ROS were significantly increased or decreased in H9C2 cells treated with DOX after miR-140-5p mimic or miR-140-5p inhibitor transfection, respectively, as well as the changed expression levels of Nrf2 and Sirt2. Furthermore, DOX- induced myocardial oxidative damage was worsened in mice treated with miR-140-5p agomir, and however the injury was alleviated in the mice administrated with miR-140-5p antagomir. Therefore, miR-140-5p plays an important role in DOX-induced cardiotoxicity by promoting myocardial oxidative stress via targeting Nrf2 and Sirt2. Our data provide novel insights for investigating DOX-induced heart injury. In addition, miR-140-5p/ Nrf2 and miR-140-5p/Sirt2 may be the new targets to treat DOX-induced cardiotoxicity.
机译:阿霉素(DOX)是一种具有强抗肿瘤作用的蒽环类抗生素,由于其心脏毒性,其临床应用受到了限制。但是,其发病机理仍未完全了解。本文的目的是探讨治疗DOX引起的心脏毒性的机制和新药物靶标。建立了H9C2细胞的体外模型以及大鼠和小鼠的体内模型。结果表明,DOX可通过调节细胞内ROS,MDA,SOD,GSH和GSH-G的水平来显着降低H9C2细胞的活力,增加CK,LDH的水平,引起大鼠和小鼠的组织病理学和心电图改变,并引发心肌氧化损伤。 Px。使用microRNA微阵列分析筛选出了由DOX引起的大鼠心脏组织中总共18种差异表达的microRNA,特别是通过选择DOX作为目标miRNA,miR-140-5p显着增加。双荧光素酶报告基因检测显示,miR-140-5p直接靶向Nrf2和Sirt2,这是因为它会影响HO-1,NQO1,Gst,GCLM,Keap1和FOXO3a的表达水平,从而增加DOX引起的心肌氧化损伤。此外,miR-140-5p模拟物或miR-140-5p抑制剂转染后,用DOX处理的H9C2细胞中的细胞内ROS水平分别显着升高或降低,以及Nrf2和Sirt2表达水平的改变。此外,在用miR-140-5p阿戈密米尔治疗的小鼠中DOX诱导的心肌氧化损伤加剧,但是在用miR-140-5p antagomir治疗的小鼠中损伤减轻。因此,miR-140-5p通过靶向Nrf2和Sirt2促进心肌氧化应激,在DOX诱导的心脏毒性中发挥重要作用。我们的数据为调查DOX诱发的心脏损伤提供了新颖的见解。此外,miR-140-5p / Nrf2和miR-140-5p / Sirt2可能是治疗DOX诱导的心脏毒性的新靶标。

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