IF 2.1 Q3 CRITICAL CARE MEDICINE
Trauma Surgery & Acute Care Open Pub Date : 2025-01-28 eCollection Date: 2025-01-01 DOI:10.1136/tsaco-2024-001559
Leslie E Neidert, Clifford G Morgan, Dominic Lonowski, Cecilia Castro, Peter J Hemond, Valeria R Lozano, Michael M Tiller, Sylvain Cardin, Jacob J Glaser
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引用次数: 0

摘要

背景:非可压缩性躯干出血(NCTH)是可预防的创伤死亡的主要原因。主动脉血管内球囊闭塞复苏术(REBOA)可稳定 NCTH,但可能使患者容易形成血栓。因此,在使用抗纤溶药氨甲环酸(TXA)的同时,必须对 REBOA 的凝血风险进行前瞻性评估。通过猪大出血模型,我们假设在使用 REBOA 的同时使用氨甲环酸(TXA)会加重凝血结果和器官损伤:32 头雄性约克夏猪接受了 30% 血容量的大出血,随机分为药物对照(VC;生理盐水)、VC+REBOA、TXA 或 TXA+REBOA。T0时,动物接受10毫升/分钟的组专用输液(GSI),然后在T10时接受500毫升全血(WB),第二次GSI为13毫升/小时,REBOA组接受1区REBOA充气。T40时,对REBOA进行放气,追加500毫升WB,并继续GSI 3小时。在整个治疗过程中测量生理、凝血和炎症参数,并进行死后组织病理学检查:在T40时REBOA放气后,REBOA组的乳酸明显高于非REBOA组,pH值、碳酸氢盐和碱过量均明显低于非REBOA组。凝血、炎症、代谢或组织病理学参数在各组间无明显差异:结论:在使用REBOA的同时使用TXA不会导致更有害的凝血结果。所有明显的变化都是REBOA缺血的预期结果,与TXA治疗无关。这表明,NCTH可以安全地使用两种出血控制方法进行治疗,而不会加重凝血结果:证据级别:不适用--基础动物研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tranexamic acid as an adjunct to resuscitative endovascular balloon occlusion of the aorta does not worsen outcomes in a porcine model of hemorrhage.

Background: Non-compressible torso hemorrhage (NCTH) represents a leading cause of preventable mortality in trauma. Resuscitative endovascular balloon occlusion of the aorta (REBOA) stabilizes NCTH but may predispose patients to thrombus generation. REBOA must therefore be prospectively evaluated for coagulation risks with concomitant usage of anti-fibrinolytic tranexamic acid (TXA). Using a porcine model of hemorrhage, it was hypothesized that TXA with REBOA would worsen coagulation outcomes and organ damage.

Materials and methods: Thirty-two male Yorkshire swine underwent 30% blood volume hemorrhage with randomization to vehicle control (VC; normal saline), VC+REBOA, TXA, or TXA+REBOA. At T0, animals received 10 mL/minute of group-specific infusion (GSI) followed at T10 by 500 mL of whole blood (WB), second GSI at 13 mL/hour, and Zone 1 REBOA inflation in REBOA groups. At T40, REBOA was deflated, with additional 500 mL WB, and continuation of GSI for 3 hours. Physiological, coagulation, and inflammatory parameters were measured throughout the protocol, with postmortem histopathology.

Results: After REBOA deflation at T40, lactate was significantly higher for the REBOA groups versus the non-REBOA groups, and pH, bicarbonate, and base excess were all significantly lower than the non-REBOA groups. There were no significant differences observed between groups in coagulation, inflammatory, metabolic, or histopathologic parameters.

Conclusions: Administration of TXA with REBOA did not cause more deleterious coagulation outcomes. All significant changes were expected results of REBOA ischemia, and not attributable to TXA treatment. This suggests NCTH can safely be treated with both hemorrhage control methods without exacerbating clotting outcomes.

Level of evidence: Not applicable-basic animal research.

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来源期刊
CiteScore
3.70
自引率
5.00%
发文量
71
审稿时长
12 weeks
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