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未分级肝素剂量对体外膜肺氧合期间补体激活和选定的细胞外囊泡群体的影响。

Effect of Unfractionated Heparin Dose on Complement Activation and Selected Extracellular Vesicle Populations during Extracorporeal Membrane Oxygenation.

机构信息

Ludwig Boltzmann Institute for Traumatology, The Research Center in Cooperation with AUVA, 1200 Vienna, Austria.

AUVA Trauma Center Salzburg, Department of Anaesthesiology and Intensive Care Medicine, Academic Teaching Hospital of the Paracelsus Medical University, 5010 Salzburg, Austria.

出版信息

Int J Mol Sci. 2024 Oct 17;25(20):11166. doi: 10.3390/ijms252011166.

Abstract

Extracorporeal membrane oxygenation (ECMO) provides critical support for patients with severe cardiopulmonary dysfunction. Unfractionated heparin (UFH) is used for anticoagulation to maintain circuit patency and avoid thrombotic complications, but it increases the risk of bleeding. Extracellular vesicles (EVs), nano-sized subcellular spheres with potential pro-coagulant properties, are released during cellular stress and may serve as potential targets for monitoring anticoagulation, particularly in thromboinflammation. We investigated the impact of UFH dose during ECMO therapy at the coagulation-inflammation interface level, focusing on complement activation and changes in circulating large EV (lEV) subsets. In a post hoc analysis of a multicenter randomized controlled trial comparing two anticoagulation management algorithms, we examined lEV levels and complement activation in 23 veno-venous-ECMO patients stratified by UFH dose. Blood samples were collected at different time points and grouped into three phases of ECMO therapy: initiation (day 1), mid (days 3-4), and late (days 6-7). Immunoassays detected complement activation, and flow cytometry analyzed lEV populations with an emphasis on mitochondria-carrying subsets. Patients receiving <15 IU/kg/h UFH exhibited higher levels of the complement activation product C5a and soluble terminal complement complex (sC5b-9). Lower UFH doses were linked to increased endothelial-derived lEVs, while higher doses were associated with elevated RBC-derived and mitochondria-positive lEVs. Our findings suggest the potential theranostic relevance of EV detection at the coagulation-inflammation interface. Further research is needed to standardize EV detection methods and validate these findings in larger ECMO patient cohorts.

摘要

体外膜肺氧合(ECMO)为严重心肺功能障碍患者提供关键支持。未分馏肝素(UFH)用于抗凝以维持回路通畅并避免血栓并发症,但会增加出血风险。细胞应激时会释放具有潜在促凝特性的纳米级细胞外囊泡(EVs),它们可能成为监测抗凝的潜在靶点,尤其是在血栓炎症中。我们研究了 ECMO 治疗期间 UFH 剂量对凝血-炎症界面水平的影响,重点关注补体激活和循环大 EV(lEV)亚群的变化。在一项比较两种抗凝管理算法的多中心随机对照试验的事后分析中,我们根据 UFH 剂量对 23 名接受静脉-静脉-ECMO 的患者进行了 lEV 水平和补体激活的检查。在 ECMO 治疗的不同时间点采集血样,并分为三个阶段:启动(第 1 天)、中期(第 3-4 天)和晚期(第 6-7 天)。免疫测定法检测补体激活,流式细胞术分析 lEV 群体,重点是携带线粒体的亚群。接受 <15 IU/kg/h UFH 的患者表现出更高水平的补体激活产物 C5a 和可溶性末端补体复合物(sC5b-9)。较低的 UFH 剂量与内皮衍生的 lEV 增加有关,而较高的剂量与 RBC 衍生的和带线粒体的 lEV 增加有关。我们的发现表明在凝血-炎症界面检测 EV 的潜在治疗相关性。需要进一步研究来标准化 EV 检测方法,并在更大的 ECMO 患者队列中验证这些发现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0b3c/11508283/3ee046f3e064/ijms-25-11166-g001.jpg

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