Carino Annarita, De Rosa Salvatore, Sorrentino Sabato, Polimeni Alberto, Sabatino Jolanda, Caiazzo Gianluca, Torella Daniele, Spaccarotella Carmen, Mongiardo Annalisa, Strangio Antonio, Filippis Carol, Indolfi Ciro
Division of Cardiology, Department of Medical and Surgical Sciences, Magna Græcia University, 88100 Catanzaro, Italy.
Division of Cardiology, Department of Medical and Surgical Sciences, Magna Græcia University, 88100 Catanzaro, Italy; URT-CNR, Department of Medicine, Consiglio Nazionale delle Ricerche, 88100 Catanzaro, Italy.
Biomed Res Int. 2016;2016:3968206. doi: 10.1155/2016/3968206. Epub 2016 Jun 6.
Background. Circulating microRNAs are appealing biomarkers to monitor several processes underlying cardiovascular diseases. Platelets are a major source for circulating microRNAs. Interestingly, the levels of specific microRNAs were reported to correlate with the level of platelet activation. The aim of the present study was to test whether the treatment with the novel antiplatelet agent, ticagrelor, is associated with modulation in the levels of key platelet-derived microRNAs. Methods and Results. Patients were randomly selected from those participating in the SHIFT-OVER study, in which we had previously evaluated the effect of the therapeutic switch from clopidogrel to ticagrelor on platelet aggregation. Circulating levels of selected microRNAs were measured before and after the therapeutic switch from a dual antiplatelet therapy including acetylsalicylic acid (ASA) and clopidogrel to the more potent ticagrelor. Interestingly, the circulating levels of miR-126 (p = 0.030), miR-223 (p = 0.044), and miR-150 (p = 0.048) were significantly reduced, while the levels of miR-96 were increased (p = 0.038). No substantial differences were observed for the remaining microRNAs. Conclusions. Switching from a dual antiplatelet treatment with clopidogrel to ticagrelor is associated with significant modulation in the circulating levels of specific microRNAs. If confirmed in larger, independent cohorts, our results pave the way for the use of circulating microRNAs as biomarkers of platelets activity in response to specific pharmacological treatments.
背景。循环微RNA是监测心血管疾病潜在多种过程的有吸引力的生物标志物。血小板是循环微RNA的主要来源。有趣的是,据报道特定微RNA的水平与血小板活化水平相关。本研究的目的是测试新型抗血小板药物替格瑞洛治疗是否与关键血小板衍生微RNA水平的调节有关。
方法与结果。患者从参与SHIFT - OVER研究的人群中随机选取,在该研究中我们之前评估了从氯吡格雷转换为替格瑞洛的治疗对血小板聚集的影响。在从包括阿司匹林(ASA)和氯吡格雷的双联抗血小板治疗转换为更强效的替格瑞洛治疗前后,测量选定微RNA的循环水平。有趣的是,miR - 126(p = 0.030)、miR - 223(p = 0.044)和miR - 150(p = 0.048)的循环水平显著降低,而miR - 96的水平升高(p = 0.038)。其余微RNA未观察到实质性差异。
结论。从氯吡格雷双联抗血小板治疗转换为替格瑞洛与特定微RNA循环水平的显著调节有关。如果在更大的独立队列中得到证实,我们的结果为将循环微RNA用作血小板对特定药物治疗反应活性生物标志物的应用铺平了道路。
