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Effects of carbon nanotube-mediated Caspase3 gene silencing on cardiomyocyte apoptosis and cardiac function during early acute myocardial infarction

机译:影响碳nanotube-mediated Caspase3基因沉默在心肌细胞凋亡和心脏在急性心肌梗死早期功能

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摘要

RNA interference (RNAi) technology can achieve efficient and specific silencing of Caspase3 gene expression, thus providing new options for anti-apoptosis treatment. However, delivering siRNA to specific cells and tissues in the body is a significant challenge. Therefore, we aim to construct a functionalized single-walled carbon nanotube (F-CNT) bound to siRNA from Caspase3. The obtained gene transfer carrier F-CNT-siCas3 not only demonstrated a good water solubility and biocompatibility, but also had a high transfection efficiency of up to 82%, which significantly downregulated the expression level of the Caspase3 gene miRNA and protein in primary cardiomyocytes. Furthermore, it was verified by in vivo experiments that Caspase3 gene silencing had obvious protective effects on myocardial cell apoptosis, ventricular remodeling, and cardiac function in Sprague-Dawley (SD) rats after coronary artery ligation. This study may provide an important theoretical basis for the application of F-CNT in vivo siRNA gene therapy to treat cardiovascular diseases.
机译:核糖核酸干扰(RNAi)技术可以实现有效的和特定的Caspase3基因的沉默表达式,从而提供新的选择抗凋亡治疗。核到特定的细胞和组织是一个重大的挑战。构造一个功能化单壁碳纳米管(F-CNT)绑定到从Caspase3核。获得的基因转移载体F-CNT-siCas3不仅表现出良好的水溶性和生物相容性,但也高转染效率高达82%,显著下调表达水平Caspase3 microrna基因和蛋白质的初选心肌细胞。体内实验,Caspase3基因沉默对心肌细胞有明显的保护作用细胞凋亡、心室重构和心脏函数Sprague-Dawley (SD)后大鼠冠状动脉结扎。一个重要的理论基础F-CNT体内核基因治疗中的应用治疗心血管疾病。

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