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Coronary Artery-Bypass-Graft Surgery Increases the Plasma Concentration of Exosomes Carrying a Cargo of Cardiac MicroRNAs: An Example of Exosome Trafficking Out of the Human Heart with Potential for Cardiac Biomarker Discovery

机译：冠状动脉搭桥手术增加了携带心脏microRNA货物的外来体的血浆浓度：外来体被运出人心脏并具有潜在的心脏生物标志物发现的例子

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INTRODUCTION: Exosome nanoparticles carry a composite cargo, including microRNAs (miRs). Cultured cardiovascular cells release miR-containing exosomes. The exosomal trafficking of miRNAs from the heart is largely unexplored. Working on clinical samples from coronary-artery by-pass graft (CABG) surgery, we investigated if: 1) exosomes containing cardiac miRs and hence putatively released by cardiac cells increase in the circulation after surgery; 2) circulating exosomes and exosomal cardiac miRs correlate with cardiac troponin (cTn), the current "gold standard" surrogate biomarker of myocardial damage. METHODS AND RESULTS: The concentration of exosome-sized nanoparticles was determined in serial plasma samples. Cardiac-expressed (miR-1, miR-24, miR-133a/b, miR-208a/b, miR-210), non-cardiovascular (miR-122) and quality control miRs were measured in whole plasma and in plasma exosomes. Linear regression analyses were employed to establish the extent to which the circulating individual miRs, exosomes and exosomal cardiac miR correlated with cTn-I. Cardiac-expressed miRs and the nanoparticle number increased in the plasma on completion of surgery for up to 48 hours. The exosomal concentration of cardiac miRs also increased after CABG. Cardiac miRs in the whole plasma did not correlate significantly with cTn-I. By contrast cTn-I was positively correlated with the plasma exosome level and the exosomal cardiac miRs. CONCLUSIONS: The plasma concentrations of exosomes and their cargo of cardiac miRs increased in patients undergoing CABG and were positively correlated with hs-cTnI. These data provide evidence that CABG induces the trafficking of exosomes from the heart to the peripheral circulation. Future studies are necessary to investigate the potential of circulating exosomes as clinical biomarkers in cardiac patients.

机译：引言：外泌体纳米颗粒可携带复合货物，包括microRNA（miR）。培养的心血管细胞释放含miR的外来体。心脏外源性miRNA的外体运输在很大程度上尚待探索。在研究冠状动脉旁路移植术（CABG）手术的临床样本时，我们调查了以下情况：1）含有心脏miR并因此推测由心脏细胞释放的外泌体在术后循环中的增加； 2）循环外泌体和外泌体心脏miR与心脏肌钙蛋白（cTn）相关，后者是目前心肌损伤的生物标志物“黄金标准”。方法和结果：在连续血浆样品中测定了外来体大小的纳米颗粒的浓度。在整个血浆和血浆外泌体中测量了心脏表达的（miR-1，miR-24，miR-133a / b，miR-208a / b，miR-210），非心血管（miR-122）和质量控制miRs 。采用线性回归分析来确定循环的单个miR，外泌体和外体心脏miR与cTn-1相关的程度。手术结束长达48小时后，血浆中心脏表达的miRs和纳米颗粒数量增加。 CABG后心脏miRs的外泌体浓度也增加。整个血浆中的心脏miR与cTn-1没有显着相关。相反，cTn-1与血浆外泌体水平和外泌体心脏miRs正相关。结论：接受CABG的患者血浆外泌体及其心脏miRs的血药浓度升高，与hs-cTnI呈正相关。这些数据提供了证据，表明CABG诱导了外来体从心脏向外周循环的运输。有必要进行进一步的研究来研究循环外泌体作为心脏病患者临床生物标志物的潜力。

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Emanueli, Costanza; Shearn, Andrew I. U.; Laftah, Abas; Fiorentino, Francesca; Reeves, Barnaby C.; Beltrami, Cristina; Mumford, Andrew; Clayton, Aled; Gurney, Mark; Shantikumar, Saran; Angelini, Gianni D.;
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4. Computationally Generated Cardiac Biomarkers: Heart Rate Patterns to Predict Death Following Coronary Attacks [C] . Chih-Chun Chia, Zeeshan Syed SIAM International Conference on Data Mining . 2011

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机译：亚洲人参的总人参皂甙通过激活Akt-eNOS信号和心脏能量相关蛋白表达，增加Langendorff系统缺血再灌注损伤大鼠心脏的冠状动脉灌注流量。
6. Coronary Artery-Bypass-Graft Surgery Increases the Plasma Concentration of Exosomes Carrying a Cargo of Cardiac MicroRNAs: An Example of Exosome Trafficking Out of the Human Heart with Potential for Cardiac Biomarker Discovery [O] . Costanza Emanueli, Andrew I. U. Shearn, Abas Laftah, -1

机译：冠状动脉搭桥手术增加了携带心脏microRNA货物的外来体的血浆浓度：外来体被运出人心脏并具有发现心脏生物标志物的潜力的例子
7. Coronary Artery-Bypass-Graft Surgery Increases the Plasma Concentration of Exosomes Carrying a Cargo of Cardiac MicroRNAs:An Example of Exosome Trafficking Out of the Human Heart with Potential for Cardiac Biomarker Discovery [O] . Emanueli Costanza, Shearn Andrew I U, Laftah Abas, 2016

机译：冠状动脉搭桥手术增加了携带心脏microRNA货物的外来体的血浆浓度：外来体从人心脏运出的实例，可能会发现心脏生物标记物

Coronary Artery-Bypass-Graft Surgery Increases the Plasma Concentration of Exosomes Carrying a Cargo of Cardiac MicroRNAs: An Example of Exosome Trafficking Out of the Human Heart with Potential for Cardiac Biomarker Discovery

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