经导管主动脉瓣置换术后血小板和单核细胞活化(pott - tavr):替格瑞洛与氯吡格雷的随机机制试验

IF 1.4 Q3 CARDIAC & CARDIOVASCULAR SYSTEMS Structural Heart Pub Date : 2023-07-01 DOI:10.1016/j.shj.2023.100182
David A. Zidar MD, PhD , Sadeer Al-Kindi MD , Chris T. Longenecker MD , Sahil A. Parikh MD , Carl B. Gillombardo MD , Nicholas T. Funderburg PhD , Steven Juchnowski , Lauren Huntington , Trevor Jenkins MD , Christopher Nmai , Michael Osnard MD , Mehdi Shishebhor DO, PhD , Steven Filby MD , Curtis Tatsuoka PhD , Michael M. Lederman MD , Eugene Blackstone MD , Guilherme Attizzani MD, PhD , Daniel I. Simon MD
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引用次数: 0

摘要

研究背景:经导管主动脉瓣置换术(TAVR)后,炎症和血栓形成通常具有机械联系,并与不良事件相关。当使用氯吡格雷时,高残余血小板反应性(HRPR)尤其常见,但其与免疫激活的相关性尚不清楚。我们试图确定嘌呤能受体P2Y12 (P2Y12)的残留活性是否在TAVR的情况下促进血栓前免疫激活。方法:这是一项随机试验,60名患者(2015年7月至2018年12月入组)在TAVR之前和之后30天内被分配到氯吡格雷(负荷300mg,每天75mg)或替格瑞洛(负荷180mg, 90 mg,每天两次)。共同主要终点是p2y12依赖性血小板活性(血小板反应单位;VerifyNow)和TAVR后1天炎症(分化簇[CD] 14+/CD16+)单核细胞比例。结果与氯吡格雷相比,随机分配替格瑞洛组的血小板抑制作用更强(血小板反应性单位中位数[四分位数范围]:234[170.0-282.3]对128.5 [86.5-156.5],p <0.001),但TAVR后1天炎症单核细胞比例相似(22.2%[18.0%-30.2%]对25.1% [22.1%-31.0%],p = 0.201)。循环单核细胞血小板聚集物、可溶性CD14水平、白细胞介素6和8水平以及d -二聚体在各治疗组之间也相似。在63%的氯吡格雷组中观察到HRPR,并与较高的炎症单核细胞比例相关。大出血事件、起搏器放置和死亡率没有因治疗分配而不同。结论氯吡格雷治疗TAVR后残留P2Y12活性普遍存在,但替格瑞洛没有显著改变血栓前免疫激活的生物标志物。在这种情况下,HRPR似乎是先天免疫激活的一个指标(而不是原因)。
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Platelet and Monocyte Activation After Transcatheter Aortic Valve Replacement (POTENT-TAVR): A Mechanistic Randomized Trial of Ticagrelor Versus Clopidogrel

Background

Inflammation and thrombosis are often linked mechanistically and are associated with adverse events after transcatheter aortic valve replacement (TAVR). High residual platelet reactivity (HRPR) is especially common when clopidogrel is used in this setting, but its relevance to immune activation is unknown. We sought to determine whether residual activity at the purinergic receptor P2Y12 (P2Y12) promotes prothrombotic immune activation in the setting of TAVR.

Methods

This was a randomized trial of 60 patients (enrolled July 2015 through December 2018) assigned to clopidogrel (300mg load, 75mg daily) or ticagrelor (180mg load, 90 mg twice daily) before and for 30 days following TAVR. Co-primary endpoints were P2Y12-dependent platelet activity (Platelet Reactivity Units; VerifyNow) and the proportion of inflammatory (cluster of differentiation [CD] 14+/CD16+) monocytes 1 day after TAVR.

Results

Compared to clopidogrel, those randomized to ticagrelor had greater platelet inhibition (median Platelet Reactivity Unit [interquartile range]: (234 [170.0-282.3] vs. 128.5 [86.5-156.5], p < 0.001), but similar inflammatory monocyte proportions (22.2% [18.0%-30.2%] vs. 25.1% [22.1%-31.0%], p = 0.201) 1 day after TAVR. Circulating monocyte-platelet aggregates, soluble CD14 levels, interleukin 6 and 8 levels, and D-dimers were also similar across treatment groups. HRPR was observed in 63% of the clopidogrel arm and was associated with higher inflammatory monocyte proportions. Major bleeding events, pacemaker placement, and mortality did not differ by treatment assignment.

Conclusions

Residual P2Y12 activity after TAVR is common in those treated with clopidogrel but ticagrelor does not significantly alter biomarkers of prothrombotic immune activation. HRPR appears to be an indicator (not a cause) of innate immune activation in this setting.

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来源期刊
Structural Heart
Structural Heart Medicine-Cardiology and Cardiovascular Medicine
CiteScore
1.60
自引率
0.00%
发文量
81
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