Platelet releasates mitigate the endotheliopathy of trauma.

IF 2.9 2区 医学 Q2 CRITICAL CARE MEDICINE
Lauren T Gallagher, Ian LaCroix, Alexander T Fields, Sanchayita Mitra, Amy Argabright, Angelo D'Alessandro, Christopher Erickson, Brenda Nunez-Garcia, Kimberly Herrera-Rodriguez, Yu Celine Chou, Benjamin W Stocker, Benjamin J Ramser, Otto Thielen, William Hallas, Christopher C Silliman, Lucy Z Kornblith, Mitchell J Cohen
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引用次数: 0

Abstract

Background: Platelets are well known for their roles in hemostasis, but they also play a key role in thromboinflammatory pathways by regulating endothelial health, stimulating angiogenesis, and mediating host defense through both contact dependent and independent signaling. When activated, platelets degranulate releasing multiple active substances. We hypothesized that the soluble environment formed by trauma platelet releasates (TPR) attenuates thromboinflammation via mitigation of trauma induced endothelial permeability and metabolomic reprogramming.

Methods: Blood was collected from injured and healthy patients to generate platelet releasates and plasma in parallel. Permeability of endothelial cells when exposed to TPR and plasma (TP) was assessed via resistance measurement by electric cell-substrate impedance sensing (ECIS). Endothelial cells treated with TPR and TP were subjected to mass spectrometry-based metabolomics.

Results: TP increased endothelial permeability, whereas TPR decreased endothelial permeability when compared with untreated cells. When TP and TPR were mixed ex vivo, TPR mitigated TP-induced permeability, with significant increase in AUC compared with TP alone. Metabolomics of TPR and TP demonstrated disrupted redox reactions and anti-inflammatory mechanisms.

Conclusion: Trauma platelet releasates provide endothelial barrier protection against TP-induced endothelial permeability. Our findings highlight a potential beneficial action of activated platelets on the endothelium in injured patients through disrupted redox reactions and increased antioxidants. Our findings support that soluble signaling from platelet degranulation may mitigate the endotheliopathy of trauma. The clinical implications of this are that activated platelets may prove a promising therapeutic target in the complex integration of thrombosis, endotheliopathy, and inflammation in trauma.

血小板释放剂可减轻创伤的内皮病变。
背景:血小板在止血方面的作用众所周知,但它们在血栓炎症通路中也发挥着关键作用,通过依赖接触信号和独立信号调节内皮健康、刺激血管生成和介导宿主防御。血小板被激活后会脱颗粒,释放出多种活性物质。我们假设,创伤血小板释放物形成的可溶性环境可通过减轻创伤诱导的内皮通透性和代谢组重构来减轻血栓炎:方法:采集受伤患者和健康患者的血液,同时生成血小板释放物和血浆。内皮细胞暴露于创伤血小板释放物(TPR)和血浆(TP)时的通透性是通过电细胞基底阻抗传感(ECIS)测量电阻来评估的。用 TPR 和 TP 处理的内皮细胞接受了基于质谱的代谢组学研究:结果:与未处理的细胞相比,TP 增加了内皮细胞的通透性,而 TPR 降低了内皮细胞的通透性。当 TP 和 TPR 在体内混合时,TPR 可减轻 TP 诱导的通透性,与单独使用 TP 相比,TPR 的 AUC 显著增加。TPR 和 TP 的代谢组学研究表明,氧化还原反应和抗炎机制被破坏:结论:TPR 可提供内皮屏障保护,防止 TP 诱导的内皮通透性。我们的研究结果凸显了活化血小板通过破坏氧化还原反应和增加抗氧化剂对受伤患者内皮的潜在有益作用。我们的研究结果支持血小板脱颗粒产生的可溶性信号可减轻创伤的内皮病变。这对临床的影响是,活化的血小板可能被证明是创伤中血栓形成、内皮病变和炎症复杂综合过程中一个有希望的治疗目标:预后/流行病学,III 级。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
6.00
自引率
11.80%
发文量
637
审稿时长
2.7 months
期刊介绍: The Journal of Trauma and Acute Care Surgery® is designed to provide the scientific basis to optimize care of the severely injured and critically ill surgical patient. Thus, the Journal has a high priority for basic and translation research to fulfill this objectives. Additionally, the Journal is enthusiastic to publish randomized prospective clinical studies to establish care predicated on a mechanistic foundation. Finally, the Journal is seeking systematic reviews, guidelines and algorithms that incorporate the best evidence available.
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