Trauma-induced coagulopathy

被引:0
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作者
Ernest E. Moore
Hunter B. Moore
Lucy Z. Kornblith
Matthew D. Neal
Maureane Hoffman
Nicola J. Mutch
Herbert Schöchl
Beverley J. Hunt
Angela Sauaia
机构
[1] Ernest E Moore Shock Trauma Center at Denver Health,Department of Surgery
[2] University of Colorado Denver,Trauma and Surgical Critical Care, Zuckerberg San Francisco General Hospital
[3] University of California San Francisco,Pittsburgh Trauma Research Center
[4] University of Pittsburgh Medical Center,Aberdeen Cardiovascular & Diabetes Centre, School of Medicine, Medical Sciences and Nutrition, Institute of Medical Sciences
[5] Duke University School of Medicine,Department of Anesthesiology and Intensive Care Medicine, AUVA Trauma Centre Salzburg
[6] Transfusion Service,Colorado School of Public Health
[7] Durham VA Medical Center,undefined
[8] University of Aberdeen,undefined
[9] Academic Teaching Hospital of the Paracelsus Medical University,undefined
[10] Salzburg and Ludwig Boltzmann Institute for Experimental and Clinical Traumatology,undefined
[11] AUVA Trauma Research Centre,undefined
[12] King’s College,undefined
[13] University of Colorado Denver,undefined
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摘要
Uncontrolled haemorrhage is a major preventable cause of death in patients with traumatic injury. Trauma-induced coagulopathy (TIC) describes abnormal coagulation processes that are attributable to trauma. In the early hours of TIC development, hypocoagulability is typically present, resulting in bleeding, whereas later TIC is characterized by a hypercoagulable state associated with venous thromboembolism and multiple organ failure. Several pathophysiological mechanisms underlie TIC; tissue injury and shock synergistically provoke endothelial, immune system, platelet and clotting activation, which are accentuated by the ‘lethal triad’ (coagulopathy, hypothermia and acidosis). Traumatic brain injury also has a distinct role in TIC. Haemostatic abnormalities include fibrinogen depletion, inadequate thrombin generation, impaired platelet function and dysregulated fibrinolysis. Laboratory diagnosis is based on coagulation abnormalities detected by conventional or viscoelastic haemostatic assays; however, it does not always match the clinical condition. Management priorities are stopping blood loss and reversing shock by restoring circulating blood volume, to prevent or reduce the risk of worsening TIC. Various blood products can be used in resuscitation; however, there is no international agreement on the optimal composition of transfusion components. Tranexamic acid is used in pre-hospital settings selectively in the USA and more widely in Europe and other locations. Survivors of TIC experience high rates of morbidity, which affects short-term and long-term quality of life and functional outcome.
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