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血小板与炎症——来自布伦内克研究及心肌梗死血小板图谱研究(PACMAN-AMI)中血小板非编码RNA含量及释放情况的见解

Platelets and inflammation-insights from platelet non-coding RNA content and release in the Bruneck study and the PACMAN-AMI trial.

作者信息

Gutmann Clemens, Barwari Temo, Schulte Christian, Theofilatos Konstantinos, Singh Bhawana, Takov Kaloyan, Suna Gonca, Chan Melissa V, Armstrong Paul C, Cassel Christian, Ueki Yasushi, Häner Jonas D, Santer Peter, Willeit Peter, Hengstenberg Christian, Räber Lorenz, Kiechl Stefan, Willeit Johann, Warner Timothy D, Mayr Manuel

机构信息

Division of Cardiology, Medical University of Vienna, Vienna, Austria.

King's British Heart Foundation Centre, King's College London, London, UK.

出版信息

Cardiovasc Res. 2025 Aug 14;121(9):1392-1406. doi: 10.1093/cvr/cvaf100.

DOI:10.1093/cvr/cvaf100
PMID:40460296
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12352307/
Abstract

AIMS

Platelets contain non-coding RNAs (ncRNAs), and their measurement may complement platelet aggregometry.

METHODS AND RESULTS

In the community-based Bruneck study (n = 338), we generated platelet-rich plasma (PRP), platelet-poor plasma (PPP), and platelets. PRP was subjected to aggregometry using various agonists and processed to platelet releasates thereafter. Releasates, PPP, and platelets underwent real-time polymerase chain reactions to measure ncRNAs. Platelet ncRNA release appeared agonist-specific, dose-dependent, and inhibited by aspirin. Collagen triggered the strongest release for most ncRNAs, whereas miR-150 was hyperresponsive to ADP, and miR-21 was hyperresponsive to arachidonic acid. Comparing the dynamic range of ncRNA release to aggregation, aggregation reached a maximum at high agonist concentrations, while ncRNAs continued to rise. Cohort-wide associations showed that inflammation parameters like neutrophil counts and C-reactive protein correlated inversely with platelet aggregation and ncRNA release. Similarly, a high leucocyte-derived RNA content in isolated platelets correlated inversely with aggregation. Inverse correlations were absent in aspirin users. Through experiments on plasma-free platelet releasates and platelets, including size-exclusion chromatography, ultracentrifugation, and degradation assays, we discovered that microRNAs and YRNAs are carried by proteins and readily released, while circular-, long non-coding-, and messenger RNAs are carried by vesicles and preferentially retained. Finally, we assessed ncRNA responses to short- and long-term dual anti-platelet therapy (DAPT) in plasma from 265 patients with acute myocardial infarction (AMI) of the PACMAN-AMI trial. Most of the DAPT effect was already achieved by 4 weeks, with a further reduction at 52 weeks, revealing a short- and long-term DAPT effect not captured by aggregometry.

CONCLUSION

Inflammation and leucocyte-derived RNAs in isolated platelets are associated with reduced platelet responses ex vivo, potentially reflecting exhaustion through pre-activation in vivo. We show that protein-bound ncRNAs are readily released from platelets, whereas vesicle-bound ncRNAs are preferentially retained. We highlight the potential of ncRNAs as biomarkers complementing aggregometry.

摘要

目的

血小板含有非编码RNA(ncRNA),对其进行检测可能补充血小板聚集检测。

方法与结果

在基于社区的布伦内克研究(n = 338)中,我们制备了富血小板血浆(PRP)、乏血小板血浆(PPP)和血小板。使用各种激动剂对PRP进行聚集检测,之后将其处理为血小板释放物。对释放物、PPP和血小板进行实时聚合酶链反应以检测ncRNA。血小板ncRNA释放表现出激动剂特异性、剂量依赖性且受阿司匹林抑制。胶原蛋白引发了大多数ncRNA的最强释放,而miR-150对ADP反应过度,miR-21对花生四烯酸反应过度。将ncRNA释放的动态范围与聚集进行比较,聚集在高激动剂浓度下达到最大值,而ncRNA持续上升。全队列关联显示,中性粒细胞计数和C反应蛋白等炎症参数与血小板聚集和ncRNA释放呈负相关。同样,分离的血小板中高白细胞衍生RNA含量与聚集呈负相关。阿司匹林使用者中不存在负相关。通过对无血浆血小板释放物和血小板进行实验,包括尺寸排阻色谱、超速离心和降解分析,我们发现微小RNA和YRNA由蛋白质携带并易于释放,而环状RNA、长链非编码RNA和信使RNA由囊泡携带并优先保留。最后,我们在PACMAN-AMI试验的265例急性心肌梗死(AMI)患者的血浆中评估了ncRNA对短期和长期双联抗血小板治疗(DAPT)的反应。大多数DAPT效应在4周时已实现,在52周时进一步降低,揭示了聚集检测未捕捉到的短期和长期DAPT效应。

结论

分离的血小板中的炎症和白细胞衍生RNA与体外血小板反应降低相关,可能反映了体内预激活导致的耗竭。我们表明蛋白质结合的ncRNA易于从血小板中释放,而囊泡结合的ncRNA优先保留。我们强调了ncRNA作为补充聚集检测的生物标志物的潜力。

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