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Anticoagulant therapy in acute lung injury: a useful tool without proper operating instruction?

机译:急性肺损伤的抗凝治疗:没有正确的操作指导的有用工具?

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摘要

Activation of the coagulation cascade resulting in alveolar fibrin deposition is recognized as a hallmark of acute lung injury (ALI). Anticoagulant treatment with recombinant human activated protein C (rhAPC) appears promising, because – like in sepsis – there is a deficiency of protein C in ALI, which is correlated with poor outcome in both syndromes. Recently in Critical Care, Waerhaug and colleagues confirmed the beneficial effects of rhAPC on pulmonary function in ovine endotoxin-induced ALI. Notably, the authors reported no differences in hemorrhage in histologic analyses between rhAPC-treated and untreated animals. However, a recently reported randomized, placebo-controlled, multicenter trial in ALI patients without severe sepsis failed to identify any differences in the number of ventilator-free days or 60 day-mortality between the rhAPC and placebo group. In addition to (or perhaps because of) the complex pathogenesis, the discrepancy between clinical and experimental results in ALI is another common feature with sepsis. The future challenge will be to transfer our theoretical knowledge adequately into daily clinical practice. Anticoagulant therapy might be a useful tool in the treatment of ALI; however the proper operating instruction remains to be defined.
机译:导致肺泡纤维蛋白沉积的凝血级联反应的激活被认为是急性肺损伤(ALI)的标志。用重组人活化蛋白C(rhAPC)进行抗凝治疗似乎很有希望,因为–与败血症一样– ALI中C蛋白缺乏,这与两种综合征的不良预后有关。 Waerhaug及其同事最近在《重症监护》中确认了rhAPC对绵羊内毒素诱导的ALI肺功能的有益作用。值得注意的是,作者报告在rhAPC治疗和未治疗的动物的组织学分析中出血没有差异。然而,最近报道的一项对没有严重败血症的ALI患者进行的随机,安慰剂对照,多中心试验未能证明rhAPC和安慰剂组之间无呼吸机天数或60天死亡率的差异。除(或可能由于)复杂的发病机制外,败血症的另一个常见特征是ALI的临床和实验结果之间的差异。未来的挑战是将我们的理论知识充分地转移到日常临床实践中。抗凝疗法可能是治疗ALI的有用工具。但是,仍然需要定义正确的操作说明。

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