Description The understanding of hemostasis physiology has been considerably advanced by models of kinetics and by the complicated interplay of cells
and soluble coagulation factors. How this physiology is currently, or will eventually, be reflected in clinical laboratory testing is
the subject of this monograph; this information is key for laboratorians to implement physiologic concepts into practical data and for
clinicians to understand the basis of and therefore correctly treat hemostatic disease. Many thousands of patients present with bleeding
disorders or bleeding complications of other diseases, and millions of individuals suffer the morbidity and mortality of thromboembolic
complications. How laboratory testing confronts the challenge of predicting different hemostatic risks and guiding therapy is the critical
subtext of the chapters in this monograph. New developments in hemostasis physiology have identified thrombin as an important, if not
central, coordinator of hemostatic function and thus a target for measurement to assess hemostatic function and risk. Whether such measurements
as endogenous thrombin potential or thromboelastography will accurately predict and/or quantitate global hemostatic function is an important
question. Modeling the clinical risks of bleeding or thromboembolism currently uses the laboratory presence or absence of particular
risk factors, but our clinical understanding of risk appears to more closely approximate a dynamic model, even within individual patients.
Therefore, testing for platelet dysfunction or comprehending the functional implications of a lupus anticoagulant may rely on our evolving
comprehension of hemostasis phyisology and perhaps require more sophisticated interpretation of clinical predictors of hemostatic risk.
This monograph aims to shed some light in these areas and promote investigation of such key hemostasis issues.
