首页> 外文期刊>Cardiovascular Diabetology >Impact of empagliflozin on subclinical left ventricular dysfunctions and on the mechanisms involved in myocardial disease progression in type 2 diabetes: rationale and design of the EMPA-HEART trial
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Impact of empagliflozin on subclinical left ventricular dysfunctions and on the mechanisms involved in myocardial disease progression in type 2 diabetes: rationale and design of the EMPA-HEART trial

机译:恩帕格列净对2型糖尿病亚临床左心室功能障碍和心肌疾病进展相关机制的影响:EMPA-HEART试验的原理和设计

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Background Asymptomatic left ventricular (LV) dysfunction is highly prevalent in type 2 diabetes patients. Unlike the other hypoglycemic drugs, SGLT2 inhibitors have shown potential benefits for reducing cardiovascular death and risk factors, aside from lowering plasma glucose levels. With this study we aim at determining whether the treatment with empagliflozin is associated with an improvement in LV functions in diabetic patients with asymptomatic LV dysfunction against Sitagliptin, which is presumably neutral on myocardial function. To determine changes in LV systolic and diastolic functions we will use s peckle - tracking echocardiography , a novel sensitive, non-invasive, bedside method allowing the calculation of LV global longitudinal strain (GLS), an index of myocardial deformability, as well as 3D echocardiography, which allows a better evaluation of LV volumes and mass. Methods The EMPA-HEART trial will be a phase III, open label, active-controlled, parallel groups, single centre, exploratory study conducted in Pisa, Italy. A cohort of 75 diabetic patients with normal LV systolic (2D-Echo EF?>?50%) and renal (eGFR sec MDRD?>?60?ml/min/1.73?mq) functions and no evidence of valvular and/or ischemic heart disease will be randomized to either Empagliflozin 10?mg/die or Sitagliptin 100?mg/die. The primary outcome is to detect a change in GLS from baseline to 1 and 6?months after treatment initiation. The secondary outcomes include changes from baseline to 6?months in 3-D Echocardiography EF, left atrial volume and E/E′, VO2max as measured at cardiopulmonary test, cardiac autonomic function tests (R–R interval during Valsalva manoeuvre, deep-breathing, lying-to-standing), and the determination of a set of plasma biomarkers aimed at studying volume, inflammation, oxidative stress, matrix remodelling, myocyte strain and injury. Discussion SGLT2 inhibitors might affect myocardial functions through mechanisms acting both directly and indirectly on the myocardium. The set of instrumental and biohumoral tests of our study might actually detect the presence and entity of empagliflozin beneficial effects on the myocardium and shed light on the mechanisms involved. Further, this study might eventually provide information to design a clinical strategy, based on echocardiography and/or biomarkers, to select the patients who might benefit more from this intervention. Trial registration EUDRACT Code 2016-0022250-10
机译:背景无症状左心室(LV)功能障碍在2型糖尿病患者中非常普遍。与其他降血糖药不同,SGLT2抑制剂除降低血浆葡萄糖水平外,还显示出降低心血管死亡和危险因素的潜在益处。通过这项研究,我们旨在确定依帕列净治疗是否与无症状西格列汀左室功能不全的糖尿病患者的左室功能改善有关,后者对心肌功能可能是中性的。为了确定左室收缩和舒张功能的变化,我们将使用斑点追踪超声心动图,一种新颖的敏感,非侵入性床旁方法,可计算左室总纵应变(GLS),心肌可变形性指数以及3D超声心动图,可以更好地评估左室容积和质量。方法EMPA-HEART试验将在意大利比萨进行的III期,开放标签,主动控制,平行小组,单中心,探索性研究中进行。一组75名糖尿病患者,其LV收缩期正常(2D-EchoEF≥50%),肾功能正常(eGFR secMDRD≥60?ml / min / 1.73?mq),且无瓣膜和/或缺血的证据心脏病将被随机分为Empagliflozin 10?mg / die或西他列汀100?mg / die。主要结果是检测治疗开始后从基线到1和6个月时GLS的变化。次要结果包括在3D超声心动图EF中从基线到6个月的变化,左心房容积和心肺测试,心脏自主神经功能测试(R–在Valsalva动作,深呼吸,卧躺期间的R间隔,以及确定一组旨在研究体积,炎症,氧化应激,基质重塑,心肌细胞应变和损伤的血浆生物标志物。讨论SGLT2抑制剂可能通过直接或间接作用于心肌的机制影响心肌功能。我们研究的一组仪器和生物体液测试实际上可能检测到依帕格列净对心肌有益的作用和存在,并阐明了所涉及的机制。此外,该研究最终可能会提供信息,以基于超声心动图和/或生物标记物设计临床策略,以选择可能从该干预中受益更多的患者。试用注册EUDRACT代码2016-0022250-10

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