Pharmacological Modulation of Long Cardiac QT Interval in Ex Vivo and in Vitro Experimental Models

M. Trotta
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Abstract

Prolongation of cardiac QT interval is one of the most dangerous consequences of hyperglycemia, acting on accumulation of reactive oxygen species and impairment of ionic pumps. Previous studies showed that the selective inhibition of the endogenous aldose reductase 2 (ALR2) activities, responsible of the oxidative heart damage following diabetes, could be a therapeutic treatment for the high glucose-related cardiac alterations. Indeed, the newly synthetized ALR2 inhibitor, the benzofuroxane derivative 5(6)-(benzo[d]thiazol-2-ylmethoxy)benzofuroxane (BF-5m), dose-dependently reduced the long cardiac QT interval in isolated rat hearts perfused with high glucose, by increasing in parallel the expression and activity of endogenous antioxidant pathways and free radical scavengers such as SIRT1 and its targets MnSOD and FOXO-1. The reduction of the oxidative stress induced by BF-5m lead also modifications of the expression of KCNQ1/KCNE1 potassium channels subunits in H9c2 cardiomyocytes exposed to high glucose, modifying the expression levels of miR-1, involved in KCNQ1 and KCNE1 expression.
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体外和体外实验模型对心脏长QT间期的药理学调节
心脏QT间期延长是高血糖最危险的后果之一,作用于活性氧的积累和离子泵的损伤。先前的研究表明,选择性抑制导致糖尿病后心脏氧化损伤的内源性醛糖还原酶2(ALR2)活性,可能是治疗高糖相关心脏改变的一种方法。事实上,新合成的ALR2抑制剂,苯并呋喃恶烷衍生物5(6)-(苯并[d]噻唑-2-基甲氧基)苯并呋喃氧烷(BF-5m),剂量依赖性地降低了用高糖灌注的分离大鼠心脏中的长心脏QT间期,通过并行增加内源性抗氧化途径和自由基清除剂如SIRT1及其靶标MnSOD和FOXO-1的表达和活性。BF-5m诱导的氧化应激的减少也导致暴露于高糖的H9c2心肌细胞中KCNQ1/KCNE1钾通道亚基的表达改变,从而改变参与KCNQ1和KCNE1表达的miR-1的表达水平。
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