脓毒症的凝血异常

Cheng-Ming Tsao , Shung-Tai Ho , Chin-Chen Wu
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引用次数: 39

摘要

随着时间的推移,脓毒症的病理生理学已经被阐明,但脓毒症可能被认为是对感染的不受控制的炎症和促凝反应。脓毒症的止血变化范围从亚临床凝血激活到急性弥散性血管内凝血(DIC)。DIC的特点是广泛的微血管血栓形成,导致多器官功能障碍/衰竭,随后消耗血小板和凝血因子,最终导致出血表现。DIC的诊断可以通过常规的实验室检查、评分算法和血栓弹性成像来进行。在这一系列事件中,凝血激活和血小板功能的抑制被推测为减轻炎症反应和改善败血症预后的有用工具。抗凝血剂进行了大量临床试验,但由于重组活化蛋白C在随机对照试验中疗效不足而退出市场,因此没有一种抗凝血剂被认为是标准治疗方法。然而,这些活化蛋白C、抗凝血酶和凝血调节蛋白试验的亚组分析表明,明显的凝血激活与抑制剂的最佳治疗效果密切相关。此外,抗血小板药物,包括乙酰水杨酸、P2Y12抑制剂和糖蛋白IIb/IIIa拮抗剂,可能降低脓毒症实验模型中的器官衰竭和死亡率,而不伴有出血风险的增加,这应该得到可靠的临床数据的支持。对于最先进的脓毒症治疗,抗凝血和抗血小板药物的疗效需要在进一步的大规模前瞻性、干预性、随机验证试验中得到证实。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Coagulation abnormalities in sepsis

Although the pathophysiology of sepsis has been elucidated with the passage of time, sepsis may be regarded as an uncontrolled inflammatory and procoagulant response to infection. The hemostatic changes in sepsis range from subclinical activation of blood coagulation to acute disseminated intravascular coagulation (DIC). DIC is characterized by widespread microvascular thrombosis, which contributes to multiple organ dysfunction/failure, and subsequent consumption of platelets and coagulation factors, eventually causing bleeding manifestations. The diagnosis of DIC can be made using routinely available laboratory tests, scoring algorithms, and thromboelastography. In this cascade of events, the inhibition of coagulation activation and platelet function is conjectured as a useful tool for attenuating inflammatory response and improving outcomes in sepsis. A number of clinical trials of anticoagulants were performed, but none of them have been recognized as a standard therapy because recombinant activated protein C was withdrawn from the market owing to its insufficient efficacy in a randomized controlled trial. However, these subgroup analyses of activated protein C, antithrombin, and thrombomodulin trials show that overt coagulation activation is strongly associated with the best therapeutic effect of the inhibitor. In addition, antiplatelet drugs, including acetylsalicylic acid, P2Y12 inhibitors, and glycoprotein IIb/IIIa antagonists, may reduce organ failure and mortality in the experimental model of sepsis without a concomitant increased bleeding risk, which should be supported by solid clinical data. For a state-of-the-art treatment of sepsis, the efficacy of anticoagulant and antiplatelet agents needs to be proved in further large-scale prospective, interventional, randomized validation trials.

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