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Diagnosis of human immunodeficiency virus associated disseminated intravascular coagulation
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Introduction
Disseminated intravascular Coagulation (DIC) is a thrombotic microangiopathy which may complicate a number of severe disease processes including sepsis. Development of microvascular thromboses results in consumption of coagulation factors and platelets and ultimate bleeding. Patients with HIV infection (PWH) often present with baseline dysregulation of the coagulation system which may increase severity and derangement of DIC presentation. Previously, we have shown that HIV is a significant risk factor for development of DIC.
Methodology
We conducted a retrospective record review of all DIC screens submitted to our tertiary coagulation laboratory in Johannesburg, South Africa, over a one year period and compared the laboratory presentation of DIC in PWH with presentation of DIC in patients without HIV infection.
Results
Over the year, 246 patients fulfilled the International Society of Thrombosis and Haemostasis (ISTH) diagnostic criteria for DIC– 108 were confirmed HIV-infected and 77 were confirmed uninfected. PWH and DIC presented at a significantly earlier age (41 vs 46 years respectively, p<0.02). The prothrombin time was significantly more prolonged (30.1s vs 26.s), the d-dimer levels were substantially higher (5.89mg/L vs 4.52mg/L) and the fibrinogen (3.92g/L vs 1.73g/L) and platelet levels (64.8 vs 114.8x109/l) were significantly lower in PWH. PWH also showed significant synthetic liver dysfunction and higher background inflammation.
Conclusion
PWH who fulfil the diagnostic criteria for DIC show significantly more dysregulation of the haemostatic system. This may reflect baseline abnormalities including endothelial dysfunction in the context of inflammation and liver dysfunction.
Title: Diagnosis of human immunodeficiency virus associated disseminated intravascular coagulation
Description:
Introduction
Disseminated intravascular Coagulation (DIC) is a thrombotic microangiopathy which may complicate a number of severe disease processes including sepsis.
Development of microvascular thromboses results in consumption of coagulation factors and platelets and ultimate bleeding.
Patients with HIV infection (PWH) often present with baseline dysregulation of the coagulation system which may increase severity and derangement of DIC presentation.
Previously, we have shown that HIV is a significant risk factor for development of DIC.
Methodology
We conducted a retrospective record review of all DIC screens submitted to our tertiary coagulation laboratory in Johannesburg, South Africa, over a one year period and compared the laboratory presentation of DIC in PWH with presentation of DIC in patients without HIV infection.
Results
Over the year, 246 patients fulfilled the International Society of Thrombosis and Haemostasis (ISTH) diagnostic criteria for DIC– 108 were confirmed HIV-infected and 77 were confirmed uninfected.
PWH and DIC presented at a significantly earlier age (41 vs 46 years respectively, p<0.
02).
The prothrombin time was significantly more prolonged (30.
1s vs 26.
s), the d-dimer levels were substantially higher (5.
89mg/L vs 4.
52mg/L) and the fibrinogen (3.
92g/L vs 1.
73g/L) and platelet levels (64.
8 vs 114.
8x109/l) were significantly lower in PWH.
PWH also showed significant synthetic liver dysfunction and higher background inflammation.
Conclusion
PWH who fulfil the diagnostic criteria for DIC show significantly more dysregulation of the haemostatic system.
This may reflect baseline abnormalities including endothelial dysfunction in the context of inflammation and liver dysfunction.
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