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首页> 外文期刊>European journal of heart failure: journal of the Working Group on Heart Failure of the European Society of Cardiology >Long‐term effects of Na + + /Ca 2+ 2+ exchanger inhibition with ORM‐11035 improves cardiac function and remodelling without lowering blood pressure in a model of heart failure with preserved ejection fraction
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Long‐term effects of Na + + /Ca 2+ 2+ exchanger inhibition with ORM‐11035 improves cardiac function and remodelling without lowering blood pressure in a model of heart failure with preserved ejection fraction

机译:Na + + / Ca 2+ 2+交换器抑制与ORM-11035的长期效应改善了心脏功能和重塑,而不会降低心力衰竭模型中的血压与保存的射血分数

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Aims Heart failure with preserved ejection fraction (HFpEF) is increasingly common but there is currently no established pharmacological therapy. We hypothesized that ORM‐11035, a novel specific Na + /Ca 2+ exchanger (NCX) inhibitor, improves cardiac function and remodelling independent of effects on arterial blood pressure in a model of cardiorenal HFpEF. Methods and results Rats were subjected to subtotal nephrectomy (NXT) or sham operation. Eight weeks after intervention, treatment for 16?weeks with ORM‐11035 (1?mg/kg body weight) or vehicle was initiated. At 24?weeks, blood pressure measurements, echocardiography and pressure–volume loops were performed. Contractile function, Ca 2+ transients and NCX‐mediated Ca 2+ extrusion were measured in isolated ventricular cardiomyocytes. NXT rats (untreated) showed a HFpEF phenotype with left ventricular (LV) hypertrophy, LV end‐diastolic pressure (LVEDP) elevation, increased brain natriuretic peptide (BNP) levels, preserved ejection fraction and pulmonary congestion. In cardiomyocytes from untreated NXT rats, early relaxation was prolonged and NCX‐mediated Ca 2+ extrusion was decreased. Chronic treatment with ORM‐11035 significantly reduced LV hypertrophy and cardiac remodelling without lowering systolic blood pressure. LVEDP [14?±?3 vs. 9?±?2?mmHg; NXT ( n ?=?12) vs. NXT?+?ORM ( n ?=?12); P ?=?0.0002] and BNP levels [71?±?12 vs. 49?±?11 pg/mL; NXT ( n ?=?12) vs. NXT?+?ORM ( n ?=?12); P ??0.0001] were reduced after ORM treatment. LV cardiomyocytes from ORM‐treated rats showed improved active relaxation and diastolic cytosolic Ca 2+ decay as well as restored NCX‐mediated Ca 2+ removal, indicating NCX modulation with ORM‐11035 as a promising target in the treatment of HFpEF. Conclusion Chronic inhibition of NCX with ORM‐11035 significantly attenuated cardiac remodelling and diastolic dysfunction without lowering systemic blood pressure in this model of HFpEF. Therefore, long‐term treatment with selective NCX inhibitors such as ORM‐11035 should be evaluated further in the treatment of heart failure.
机译:AIMS与保存的射血分数(HFPEF)的心力衰竭越来越普遍,但目前没有建立的药理学疗法。我们假设ORM-11035,一种新的特异性Na + / Ca 2+交换剂(NCX)抑制剂,改善心脏函数和重塑,与心血管HFPEF模型的动脉血压的影响无关。方法和结果对大鼠进行小肾切除术(NXT)或假手术。干预后八周,启动了16个?60周的16〜数周(1?Mg / kg体重)或载体。在24个?周,进行血压测量,超声心动图和压力体积回路。在分离的心室心肌细胞中测量收缩功能,Ca 2+瞬变和NCX介导的Ca 2+挤出。 NXT大鼠(未处理)显示HFPEF表型,左心室(LV)肥大,LV端舒张压(LVEDP)升高,增加脑利钠肽(BNP)水平,保存的射血分数和肺充血。在来自未处理的NXT大鼠的心肌细胞中,延长早期弛豫,并且NCX介导的Ca 2+挤出减少。慢性治疗ORM-11035显着降低了LV肥大和心脏重塑而不降低收缩压。 lvedp [14?±3 vs. 9?±2?mmhg; nxt(n?=?12)与nxt?+?orm(n?=?12); p?= 0.0002]和BNP水平[71?±12与49?±11 pg / ml; nxt(n?=?12)与nxt?+?orm(n?=?12); P?α&Δ01]在治疗后减少。来自ORM处理的大鼠的LV心肌细胞显示出改善的活性松弛和舒张胞嘧啶Ca 2+衰减以及恢复的NCX介导的Ca 2+去除,表明NCX调节与ORM-11035作为治疗HFPEF的有希望的靶标。结论NCX与ORM-11035的NCX慢性抑制显着减弱了心脏重塑和舒张功能障碍,而不是降低该型HFPEF模型的全身血压。因此,应在治疗心力衰竭的情况下进一步评估具有选择性NCX抑制剂的长期处理,例如ORM-11035。

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