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首页> 外文期刊>Circulation journal >Q50, an iron-chelating and zinc-complexing agent, improves cardiac function in rat models of ischemia/reperfusion-induced myocardial injury
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Q50, an iron-chelating and zinc-complexing agent, improves cardiac function in rat models of ischemia/reperfusion-induced myocardial injury

机译:Q50,一种铁螯合和锌络合剂,改善了大鼠缺血/再灌注诱导的心肌损伤的大鼠模型中的心功能

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摘要

Background: Reperfusion of ischemic myocardium may contribute to substantial cardiac tissue damage, but the addition of iron chelators, zinc or zinc complexes has been shown to prevent heart from reperfusion injury. We investigated the possible beneficial effects of an iron-chelating and zinc-complexing agent, Q50, in rat models of ischemia/reperfusion (I/R)-induced myocardial infarction and on global reversible myocardial I/R injury after heart transplantation. Methods and Results: Rats underwent 45-min myocardial ischemia by left anterior descending coronary artery ligation followed by 24 h reperfusion. Vehicle or Q50 (10 mg/kg, IV) were given 5 min before reperfusion. In a heart transplantation model, donor rats received vehicle or Q50 (30 mg/kg, IV) 1 h before the onset of ischemia. In myocardial infarcted rats, increased left ventricular end-systolic and end-diastolic volumes were significantly decreased by Q50 post treatment as compared with the sham group. Moreover, in I/R rat hearts, the decreased dP/dtmax and load-independent contractility parameters were significantly increased after Q50. However, Q50 treatment did not reduce infarct size or have any effect on increased plasma cardiac troponin-T-levels. In the rat model of heart transplantation, 1 h after reperfusion, decreased left ventricular systolic pressure, dP/dtmax, dP/dtmin and myocardial ATP content were significantly increased and myocardial protein expression of superoxide dismutase-1 was upregulated after Q50 treatment. Conclusions: In 2 experimental models of I/R, administration of Q50 improved myocardial function. Its mechanisms of action implicate in part the restoration of myocardial high-energy phosphates and upregulation of antioxidant enzymes. (Circ J 2013; 77: 1817 - 1826).
机译:背景技术:缺血性心肌的再灌注可能有助于大量心脏组织损伤,但是已经显示了加入铁螯合剂,锌或锌络合物以防止心脏再灌注损伤。我们调查了铁螯合和锌络合剂,Q50在大鼠缺血/再灌注(I / R)的大鼠模型中可能的有益效果 - 诱导心肌梗死和心脏移植后全局可逆心肌I / R损伤。方法和结果:大鼠通过左前期下降冠状动脉结扎后进行45分钟的心肌缺血,然后进行24小时再灌注。在再灌注前5分钟给出车辆或Q50(10mg / kg,iv)。在心脏移植模型中,供体大鼠在缺血开始之前接受载体或Q50(30mg / kg,iv)1小时。在心肌梗死的大鼠中,随着假组的Q50后治疗,Q50后处理增加,左心室最终收缩量和末端舒张性体积的增加显着降低。此外,在I / R大鼠的心中,在Q50之后,在I / R大鼠心中,降低的DP / DTmax和载荷无合的收缩性参数显着增加。然而,Q50治疗没有降低梗塞大小或对增加的血浆心肌肌钙蛋白-T水平有任何影响。在RAT模型的心脏移植模型中,再灌注后1小时,左心室收缩压,DP / DTMAX,DP / DTMIN和心肌ATP含量显着增加,并且在Q50处理后上调超氧化物歧化酶-1的心肌蛋白表达。结论:在I / R的2种实验模型中,Q50的施用改善了心肌功能。其作用机制部分地涉及恢复心肌高能量磷酸盐和抗氧化酶的上调。 (2013年CIRC; 77:1817 - 1826)。

著录项

  • 来源
    《Circulation journal》 |2013年第7期|共10页
  • 作者

    KorkmazS.; BarnuczE.; LoganathanS.; LiS.; RadovitsT.; HegedusP.; ZubarevichA.; HirschbergK.; WeymannA.; PuskásL.G.; ózsváriB.; FaragóN.; KanizsaiI.; FábiánG.; GyurisM.; MerkelyB.; KarckM.; SzabóC.; SzabóG.;

  • 作者单位

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany Heart Center;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Heart Center Semmelweis University Budapest Hungary;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany Heart Center;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Avidin Ltd Szeged Hungary Avicor Ltd Szeged Hungary Laboratory for Functional Genomics;

    Avidin Ltd Szeged Hungary;

    Avidin Ltd Szeged Hungary Laboratory for Functional Genomics Department of Genetics Biological;

    Avidin Ltd Szeged Hungary;

    Avicor Ltd Szeged Hungary;

    Avidin Ltd Szeged Hungary;

    Heart Center Semmelweis University Budapest Hungary;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

    Department of Anesthesiology University of Texas Medical Branch TX United States;

    Department of Cardiac Surgery University of Heidelberg Heidelberg Germany;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 心脏、血管(循环系)疾病;
  • 关键词

    Antioxidants; Ischemia/reperfusion; Myocardial infarction; Transplantation;

    机译:抗氧化剂;缺血/再灌注;心肌梗塞;移植;

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