Traumatic bleeding and mortality in mice are intensified by iron deficiency anemia and can be rescued with tranexamic acid

IF 3.4 3区医学 Q2 HEMATOLOGY

Research and Practice in Thrombosis and Haemostasis Pub Date : 2024-08-01 DOI:10.1016/j.rpth.2024.102543

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Abstract

Background

Clinical evidence suggests that anemia exacerbates traumatic bleeding and worsens outcomes.

Objectives

To study the influence of iron deficiency anemia on traumatic bleeding, coagulopathy, and mortality.

Methods

C57BL/6J mice received an iron-deficient diet (8 weeks; ±1 mg intraperitoneal iron dextran 2 weeks before trauma). Control mice received a normal diet. Iron deficiency anemia was confirmed by hematocrit, red cell indices, and liver iron. Mice received saline or tranexamic acid (TXA; 10 mg/kg) just before liver laceration. Blood loss, coagulopathy (activated partial thromboplastin time, factor [F]II, FV, FVIII, FX, and fibrinogen), D-dimer, thrombin-antithrombin complexes, and plasmin-alpha-2-antiplasmin complexes were analyzed at 15 and 60 minutes, and a cytokine panel was performed at 60 minutes and 6 hours after trauma. Survival was monitored for 7 days.

Results

Compared with nonanemic mice, anemic mice had lower hematocrit and hepatic iron content. Anemic mice experienced higher blood loss compared with nonanemic mice, which was reduced by TXA. Both groups developed traumatic coagulopathy characterized by activated partial thromboplastin time prolongation, thrombin-antithrombin complex formation, and depletion of FV, FVIII, and fibrinogen. TXA corrected the coagulopathy. However, plasmin-alpha-2-antiplasmin complex formation and D-dimers, markers of fibrinolysis, were higher in anemic mice and were not corrected by TXA. Seven-day survival was low in anemic mice, and rescued by TXA, but high in nonanemic mice without additional improvement by TXA. Among cytokines, only interleukin-6 increased, which was prevented by TXA most notably in anemic mice.

Conclusion

These observations provide first and critical proof-of-principle evidence that anemia accelerates traumatic bleeding and increases mortality, which could be rescued by anemia correction (parenteral iron) or periprocedural TXA.

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缺铁性贫血会加剧小鼠的创伤性出血和死亡率，氨甲环酸可以缓解这种情况

研究缺铁性贫血对创伤出血、凝血病和死亡率的影响。方法 C57BL/6J 小鼠接受缺铁饮食（8 周；创伤前 2 周腹腔注射 ±1 毫克右旋糖酐铁）。对照组小鼠的饮食正常。缺铁性贫血由血细胞比容、红细胞指数和肝铁证实。小鼠在肝脏撕裂前接受生理盐水或氨甲环酸（TXA；10 毫克/千克）治疗。分别在15分钟和60分钟时分析失血量、凝血功能（活化部分凝血活酶时间、因子[F]II、FV、FVIII、FX和纤维蛋白原）、D-二聚体、凝血酶-抗凝血酶复合物和凝血酶-α-2-抗凝血酶复合物，并在创伤后60分钟和6小时时进行细胞因子检测。结果与非贫血小鼠相比，贫血小鼠的血细胞比容和肝铁含量较低。与非贫血小鼠相比，贫血小鼠的失血量更高，而 TXA 可减少失血量。两组小鼠都出现了创伤性凝血病，其特点是活化部分凝血活酶时间延长、凝血酶-抗凝血酶复合物形成以及 FV、FVIII 和纤维蛋白原耗竭。TXA 可纠正凝血病症。然而，贫血小鼠的凝血酶-α-2-抗凝血酶复合物形成和 D-二聚体（纤溶标志物）较高，且 TXA 无法纠正。贫血小鼠的七天存活率较低，TXA 可挽救贫血小鼠的七天存活率，但非贫血小鼠的七天存活率较高，TXA 无法改善贫血小鼠的七天存活率。在细胞因子中，只有白细胞介素-6 增高，而贫血小鼠的白细胞介素-6 增高最明显地受到 TXA 的抑制。结论：这些观察结果首次提供了重要的原则性证据，证明贫血会加速创伤性出血并增加死亡率，而贫血纠正（肠外铁剂）或围手术期 TXA 可以挽救这种情况。

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