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Nanosecond pulsed platelet‐rich plasma (nsPRP) improves mechanical and electrical cardiac function following myocardial reperfusion injury

机译:纳秒脉冲富血小板血浆(nsPRP)改善心肌再灌注损伤后的机械和电心功能

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摘要

Ischemia and reperfusion (I/R) of the heart is associated with biochemical and ionic changes that result in cardiac contractile and electrical dysfunction. In rabbits, platelet‐rich plasma activated using nanosecond pulsed electric fields (nsPRP) has been shown to improve left ventricular pumping. Here, we demonstrate that nsPRP causes a similar improvement in mouse left ventricular function. We also show that nsPRP injection recovers electrical activity even before reperfusion begins. To uncover the mechanism of nsPRP action, we studied whether the enhanced left ventricular function in nsPRP rabbit and mouse hearts was associated with increased expression of heat‐shock proteins and altered mitochondrial function under conditions of oxidative stress. Mouse hearts underwent 30 min of global ischemia and 1 h of reperfusion in situ. Rabbit hearts underwent 30 min of ischemia in vivo and were reperfused for 14 days. Hearts treated with nsPRP expressed significantly higher levels of Hsp27 and Hsp70 compared to hearts treated with vehicle. Also, pretreatment of cultured H9c2 cells with nsPRP significantly enhanced the “spare respiratory capacity (SRC)” also referred to as “respiratory reserve capacity” and ATP production in response to the uncoupler FCCP. These results suggest a cardioprotective effect of nsPRP on the ischemic heart during reperfusion.
机译:心脏的缺血和再灌注(I / R)与导致心脏收缩和电功能障碍的生化和离子变化有关。在兔子中,已证明使用纳秒脉冲电场(nsPRP)激活的富含血小板的血浆可改善左心室泵血。在这里,我们证明nsPRP会导致小鼠左心室功能的类似改善。我们还显示,nsPRP注射甚至在再灌注开始之前就可以恢复电活动。为了揭示nsPRP作用的机制,我们研究了在氧化应激条件下nsPRP兔和小鼠心脏左心室功能增强是否与热休克蛋白表达增加和线粒体功能改变有关。小鼠心脏经历了整体缺血30分钟和原位再灌注1小时。兔心脏在体内经历30分钟的局部缺血,并再灌注14天。与用媒介物治疗的心脏相比,使用nsPRP治疗的心脏表达的Hsp27和Hsp70水平明显更高。同样,用nsPRP预处理培养的H9c2细胞可显着增强“备用呼吸能力(SRC)”,也称为“呼吸储备能力”和对解偶联剂FCCP的ATP产生。这些结果表明nsPRP在再灌注期间对缺血心脏的心脏保护作用。

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