Currently, information on hypercoagulability can be achieved directly- through measuring the enzymatic forms of coagulation zymogens generated during coagulation activation-or indirectly-through measuring the activation peptides generated when zymogens are activated or the enzyme-inhibitor complexes formed by inhibition of the enzymes by their plasmatic inhibitors. On the basis of published results, markers of activated coagulation are considered useful for investigating mechanisms that regulate hemostasis. They can also be used to better characterize patients at increased thrombotic risk. However, they should be considered indices of hypercoagulability, not of the risk of thrombosis, until prospective studies can demonstrate that alterations of these markers can predict the occurrence of thrombosis. For diagnosing acute thrombosis, their usefulness is questionable; they are less effective than markers of fibrinolysis activation such as the D-dimer. Finally, their use to monitor anticoagulant treatment is still premature and needs investigation in well-designed clinical studies.

Markers of activated coagulation and their usefulness in the clinical laboratory / A. Tripodi, P.M. Mannucci. - In: CLINICAL CHEMISTRY. - ISSN 0009-9147. - 42:5(1996), pp. 664-669.

Markers of activated coagulation and their usefulness in the clinical laboratory

A. Tripodi
Primo
;
1996

Abstract

Currently, information on hypercoagulability can be achieved directly- through measuring the enzymatic forms of coagulation zymogens generated during coagulation activation-or indirectly-through measuring the activation peptides generated when zymogens are activated or the enzyme-inhibitor complexes formed by inhibition of the enzymes by their plasmatic inhibitors. On the basis of published results, markers of activated coagulation are considered useful for investigating mechanisms that regulate hemostasis. They can also be used to better characterize patients at increased thrombotic risk. However, they should be considered indices of hypercoagulability, not of the risk of thrombosis, until prospective studies can demonstrate that alterations of these markers can predict the occurrence of thrombosis. For diagnosing acute thrombosis, their usefulness is questionable; they are less effective than markers of fibrinolysis activation such as the D-dimer. Finally, their use to monitor anticoagulant treatment is still premature and needs investigation in well-designed clinical studies.
anticoagulants; autoimmune disorders; cardiopulmonary bypass; coagulation cascade; hemostasis; peptides; systemic lupus erythematosus; thrombomodulin; thrombophilia; thrombosis
Settore BIO/12 - Biochimica Clinica e Biologia Molecolare Clinica
Settore MED/09 - Medicina Interna
Settore MED/15 - Malattie del Sangue
1996
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/213436
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