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Tranexamic acid modulates the immune response and reduces postsurgical infection rates

机译:氨甲环酸调节免疫反应并降低术后感染率

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摘要

Tranexamic acid (TXA) is an antifibrinolytic agent that blocks plasmin formation. Because plasmin is known to promote inflammatory and immunosuppressive responses, we explored the possibility that plasmin-mediated immunosuppression in patients undergoing cardiac surgery can be directly reversed by TXA and decrease postoperative infection rates. The modulatory effect of TXA on inflammatory cytokine levels and on innate immune cell activation were evaluated with multiplex enzyme-linked immunosorbent assay and flow cytometry, respectively. Postoperative infection rates were determined in patients undergoing cardiac surgery and randomized to TXA (ACTRN12605000557639; ). We demonstrate that TXA-mediated plasmin blockade modulates the immune system and reduces surgery-induced immunosuppression in patients following cardiac surgery. TXA enhanced the expression of immune-activating markers while reducing the expression of immunosuppressive markers on multiple myeloid and lymphoid cell populations in peripheral blood. TXA administration significantly reduced postoperative infection rates, despite the fact that patients were being administered prophylactic antibiotics. This effect was independent of the effect of TXA at reducing blood loss. TXA was also shown to exert an immune-modulatory effect in healthy volunteers, further supporting the fibrin-independent effect of TXA on immune function and indicating that baseline plasmin levels contribute to the regulation of the immune system in the absence of any comorbidity or surgical trauma. Finally, the capacity of TXA to reduce infection rates, modulate the innate immune cell profile, and generate an antifibrinolytic effect overall was markedly reduced in patients with diabetes, demonstrating for the first time that the diabetic condition renders patients partially refractory to TXA.
机译:氨甲环酸(TXA)是一种抗纤维蛋白溶解剂,可阻止纤溶酶的形成。由于已知纤溶酶可促进炎症和免疫抑制反应,因此我们探讨了TXA可直接逆转接受心脏手术的患者中纤溶酶介导的免疫抑制并降低术后感染率的可能性。通过多重酶联免疫吸附试验和流式细胞术分别评估了TXA对炎症细胞因子水平和对先天免疫细胞活化的调节作用。确定接受心脏手术的患者的术后感染率,并随机分配至TXA(ACTRN12605000557639;)。我们证明,TXA介导的纤溶酶阻断可调节免疫系统并减少心脏手术后患者的手术诱导的免疫抑制。 TXA增强了免疫激活标志物的表达,同时降低了外周血中多个髓样和淋巴样细胞群体上免疫抑制标志物的表达。尽管患者正在使用预防性抗生素,TXA的使用仍显着降低了术后感染率。该作用与TXA减少失血的作用无关。还显示TXA在健康志愿者中发挥免疫调节作用,进一步支持TXA对免疫功能的非纤维蛋白依赖性作用,并表明在没有任何合并症或手术创伤的情况下,基线纤溶酶水平有助于调节免疫系统。 。最后,在糖尿病患者中,TXA降低感染率,调节先天免疫细胞谱以及产生抗纤维蛋白溶解作用的能力明显降低,这首次表明糖尿病使患者对TXA不能部分耐受。

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