D-二聚体和纤维蛋白降解产物损害血小板信号转导:血浆 D-二聚体是创伤期间血小板功能障碍的预测因子和介质。
D-Dimer and Fibrin Degradation Products Impair Platelet Signaling: Plasma D-Dimer Is a Predictor and Mediator of Platelet Dysfunction During Trauma.
机构信息
Department of Chemical and Biomolecular Engineering, Institute for Medicine and Engineering, University of Pennsylvania, Philadelphia, PA.
Penn Acute Research Collaboration (PARC), Department of Trauma, Surgical Critical Care, and Emergency Surgery, University of Pennsylvania, Philadelphia, PA.
出版信息
J Appl Lab Med. 2020 Nov 1;5(6):1253-1264. doi: 10.1093/jalm/jfaa047.
BACKGROUND
Platelet dysfunction often accompanies trauma-induced coagulopathy. Because soluble fibrin impairs platelet glycoprotein VI (GPVI) signaling and platelets of trauma patients can display impaired calcium mobilization, we explored the role of fibrinolysis on platelet dysfunction during trauma.
METHODS
Convulxin-induced GPVI calcium mobilization was investigated in healthy platelet-rich plasma (PRP) pretreated with thrombin and tissue plasminogen activator (tPA). Blood samples from healthy participants (n = 7) and trauma patients (n = 22) were tested for platelet calcium mobilization, plasma D-dimer, platelet D-dimer binding (via flow cytometry), and platelet lumi-aggregometry.
RESULTS
For healthy platelets, maximal platelet dysfunction was observed when cross-linked soluble fibrin (no tPA) or cross-linked fibrin degradation products (FDPs) were generated in suspension before convulxin stimulation. Lack of fibrin polymerization (inhibited by Gly-Pro-Arg-Pro [GPRP]) or lack of factor XIIIa cross-linking (T101-inhibited) restored GPVI signaling, whereas non-cross-linked FDPs only partially blocked signaling induced by convulxin. In addition, D-dimer added to healthy PRP impaired platelet aggregation and dense granule release induced by various agonists. Plasma D-dimer level was strongly correlated (R = 0.8236) with platelet dysfunction as measured by platelet calcium mobilization induced with various agonists. By 48 to 120 h after trauma, plasma D-dimer levels declined, and platelet function increased significantly but not to healthy levels. Trauma platelets displayed elevated D-dimer binding that was only partially reduced by αIIbβ3-inhibitor GR144053. After 60-minute incubation, washed healthy platelets resuspended in plasma from trauma patients captured approximately 10 000 D-dimer equivalents per platelet.
CONCLUSIONS
During trauma, D-dimer and FDPs inhibit platelets, potentially via GPVI and integrin αIIbβ3 engagement, contributing to a fibrinolysis-dependent platelet loss-of-function phenotype.
背景
血小板功能障碍常伴有创伤诱导的凝血病。由于可溶性纤维蛋白可损害血小板糖蛋白 VI(GPVI)信号,且创伤患者的血小板可能显示钙动员受损,因此我们研究了纤溶在创伤期间血小板功能障碍中的作用。
方法
在凝血酶和组织纤溶酶原激活物(tPA)预处理的健康富含血小板血浆(PRP)中,研究了 convulxin 诱导的 GPVI 钙动员。测试了健康参与者(n=7)和创伤患者(n=22)的血小板钙动员、血浆 D-二聚体、血小板 D-二聚体结合(通过流式细胞术)和血小板发光聚集。
结果
对于健康血小板,当 convulxin 刺激前在悬浮液中生成交联可溶性纤维蛋白(无 tPA)或交联纤维蛋白降解产物(FDPs)时,观察到最大的血小板功能障碍。缺乏纤维蛋白聚合(由 Gly-Pro-Arg-Pro [GPRP] 抑制)或缺乏因子 XIIIa 交联(T101 抑制)恢复了 GPVI 信号,而非交联的 FDP 仅部分阻断 convulxin 诱导的信号。此外,D-二聚体添加到健康 PRP 中会损害各种激动剂诱导的血小板聚集和致密颗粒释放。血小板钙动员诱导的各种激动剂诱导的血小板功能障碍与血浆 D-二聚体水平呈强相关性(R=0.8236)。创伤后 48 至 120 小时,血浆 D-二聚体水平下降,血小板功能显著增加,但未恢复到健康水平。创伤血小板显示出升高的 D-二聚体结合,仅部分被 αIIbβ3 抑制剂 GR144053 降低。孵育 60 分钟后,重悬在创伤患者血浆中的洗涤健康血小板每血小板捕获约 10000 D-二聚体当量。
结论
在创伤期间,D-二聚体和 FDP 通过 GPVI 和整合素 αIIbβ3 结合抑制血小板,可能导致依赖纤溶的血小板功能丧失表型。
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