• Br. J. Haematol. · Oct 2006

    Global tests of haemostasis in critically ill patients with severe sepsis syndrome compared to controls.

    • Peter W Collins, Luis I Macchiavello, Sarah J Lewis, Nichola J Macartney, Anton G Saayman, Roger Luddington, Trevor Baglin, and George P Findlay.
    • Department of Haematology, School of Medicine, Cardiff University and University Hospital of Wales, Cardiff, UK. peter.collins@cardffandvale.wales.nhs.uk
    • Br. J. Haematol. 2006 Oct 1; 135 (2): 220-7.

    AbstractHaemostatic changes in septic patients are complex, with both procoagulant and anticoagulant changes. Thirty-eight patients with severe sepsis and 32 controls were investigated by coagulation screens, individual factor assays, calibrated automated thrombography (CAT), whole blood low-dose-tissue factor activated (LD-TFA) Rotem and LD-TFA waveform analysis. Thirty-six of 38 patients had an abnormal coagulation screen. The mean levels of factors II, V (P < 0.05), VII, X, XI and XII, antithrombin and protein C (P < 0.01) was decreased in sepsis compared with controls. The mean factor VIII and fibrinogen level (P < 0.001) was increased. CAT in platelet rich and poor plasma showed a prolonged lag time (P < 0.02), decreased peak thrombin (P < 0.02) and delayed time to peak thrombin (P < 0.001) in sepsis patients, however, the endogenous thrombin potential was equivalent in sepsis and controls. In LD-TFA Rotem, septic patients had delayed clot times (P = 0.04) but an increased maximum velocity of clot formation (P < 0.01) and area under the clot elasticity curve (P < 0.01). LD-TFA waveform analysis showed a delayed onset time but an increased rate of clot formation (P < 0.005). In conclusion, global tests of haemostasis suggest that in this patient group, activation of haemostasis is delayed but once initiated thrombin generation and clot formation are normal or enhanced.

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