Your search keyword '"WATERS, E. K."' showing total 2 results

1. Modulation of the activated protein C pathway in severe haemophilia A patients: The effects of thrombomodulin and a factor V-stabilizing fab.

Author

Brophy, D. F., Martin, E. J., Mohammed, B. M., Barrett, J. C., Kuhn, J. G., Nolte, M. E., Wiinberg, B., Holmberg, H. L., Lund, J., Salbo, R., and Waters, E. K.

Subjects

THROMBOMODULIN, ACTIVATED protein C resistance, HEMOSTASIS, IMMUNOGLOBULINS, HEMORRHAGE

Abstract

Introduction The thrombomodulin (TM)/activated protein C (APC) system is a key regulator of haemostasis, limiting amplification and propagation of the formed blood clot to the injury site. Dampening APC's inhibition of factor V (FV) and factor VIII (FVIII) may be a future strategy in developing next-generation therapeutic targets for haemophilia treatment. Aims To determine ex vivo the respective concentration-dependent effects of TM and a FV-stabilizing Fab on the APC regulatory pathway in severe FVIII-deficient blood and plasma. Methods Ten severe haemophilia A subjects and one healthy control were enrolled. Blood was spiked with TM (0, 1, 2.5, 5, 10, 20.0 nmol/L) and FV-stabilizing Fab (0, 3, 15, 65, 300 nmol/L). The respective effects were compared to FVIII concentrations of 3- and 10% using rotational thromboelastometry clotting time (CT) and thrombin generation analysis (TGA). Results With 1 and 2.5 nmol/L TM, 5% FVIII resulted in CT similar to the absence of TM, suggesting it completely reversed the effect of APC. Increasing TM concentrations also reduced peak thrombin generation and ETP. The addition of 300 nmol/L FV-stabilizing Fab returned CT to nearly baseline, but for most subjects was less than the effects of 3- or 10% FVIII. The FV-stabilizing Fab produced similar or greater thrombin generation compared to samples with 3- or 10% FVIII. Conclusions The FV-stabilizing Fab resulted in enhanced CT and TGA parameters consistent with FVIII levels of 3- and 10%. Additional studies need to further characterize how modulating the APC pathway may prove beneficial in developing new haemophilia drug targets. [ABSTRACT FROM AUTHOR]

Published

2017

2. Concizumab, an anti-tissue factor pathway inhibitor antibody, induces increased thrombin generation in plasma from haemophilia patients and healthy subjects measured by the thrombin generation assay.

Author

Waters, E. K., Sigh, J., Friedrich, U., Hilden, I., and Sørensen, B. B.

Subjects

*HEMOPHILIA treatment, *THERAPEUTIC use of monoclonal antibodies, *THROMBOPLASTIN, *IMMUNOGLOBULINS, *THROMBIN

Abstract

Aims Concizumab, a humanized monoclonal antibody against tissue factor pathway inhibitor ( TFPI), is being developed as a subcutaneously (s.c.) administered treatment for haemophilia. It demonstrated a concentration-dependent procoagulant effect in functional TFPI assays; however, global haemostatic assays, such as the thrombin generation assay ( TGA), offer a more complete picture of coagulation. We investigated how concizumab affects thrombin generation following ex vivo spiking in plasma from haemophilia patients using the TGA, and if the assay can detect the effect of multiple s.c. concizumab doses in healthy subjects. Methods For the ex vivo spiking study, platelet-poor plasma ( PPP) from 18 patients with severe haemophilia was spiked with 0.001-500 n m concizumab. For the multiple-dosing study, four healthy males received concizumab 250 μg kg−1 s.c. every other day for eight doses; blood was collected before and after dosing and processed into PPP. In both studies, thrombin generation was measured using a Calibrated Automated Thrombogram® system with 1 p m tissue factor. Results In spiked samples from haemophilia patients, peak thrombin and endogenous thrombin potential ( ETP) increased concentration dependently, reaching near-normal levels at concizumab concentrations >10 n m. Repeated s.c. doses of concizumab in healthy subjects increased both peak thrombin and ETP; these effects were sustained throughout the dosing interval. Conclusions Thrombin generation assay demonstrated increased thrombin generation with concizumab after ex vivo spiking of haemophilia plasma and multiple s.c. doses in healthy subjects, supporting both the utility of the TGA in evaluating concizumab treatment and the potential of s.c. concizumab as a novel haemophilia therapy. [ABSTRACT FROM AUTHOR]

Published

2017