Tissue Factor-Independent Coagulation Correlates with Clinical Phenotype in Factor XI Deficiency and Replacement Therapy

Debora Bertaggia Calderara; Maxime G Zermatten; Alessandro Aliotta; Ana P Batista Mesquita Sauvage; Vanessa Carle; Christian Heinis; Lorenzo Alberio

doi:10.1055/s-0040-1715899

Tissue Factor-Independent Coagulation Correlates with Clinical Phenotype in Factor XI Deficiency and Replacement Therapy

Thromb Haemost. 2021 Feb;121(2):150-163. doi: 10.1055/s-0040-1715899. Epub 2020 Sep 13.

Authors

Debora Bertaggia Calderara¹, Maxime G Zermatten¹, Alessandro Aliotta¹, Ana P Batista Mesquita Sauvage¹, Vanessa Carle², Christian Heinis², Lorenzo Alberio¹

Affiliations

¹ Division of Hematology and Central Hematology Laboratory, Lausanne University Hospital (CHUV), University of Lausanne (UNIL), Lausanne, Switzerland.
² Institute of Chemical Sciences and Engineering, Ecole polytechnique fédérale de Lausanne (EPFL), Lausanne, Switzerland.

PMID: 32920807
DOI: 10.1055/s-0040-1715899

Abstract

Background: In factor XI (FXI) deficiency, bleeding cannot be predicted by routine analyses. Since FXI is involved in tissue factor (TF)-independent propagation loop of coagulation, we hypothesized that investigating the spatiotemporal separated phases of coagulation (TF-dependent and -independent) could improve diagnostics.

Objectives: This article investigates the correlation of parameters describing TF-dependent and -independent coagulation with the clinical phenotype of FXI deficiency and their ability to assess hemostasis after FXI replacement.

Methods: We analyzed: (1) plasma from healthy controls (n = 53); (2) normal plasma (n = 4) spiked with increasing concentrations of a specific FXI inhibitor (C7P); (3) plasma from FXI-deficient patients (n = 24) with different clinical phenotypes (13 bleeders, 8 non-bleeders, 3 prothrombotics); (4) FXI-deficient plasma spiked with FXI concentrate (n = 6); and (5) plasma from FXI-deficient patients after FXI replacement (n = 7). Thrombin generation was measured with the reference method calibrated automated thrombogram and with Thrombodynamics (TD), a novel global assay differentiating TF-dependent and -independent coagulation.

Results: C7P dose-dependently decreased FXI activity, prolonged activated partial thromboplastin time, and hampered TF-independent coagulation. In FXI-deficient bleeders, TD parameters describing TF-independent propagation of coagulation and fibrin clot formation were reduced compared with controls and FXI-deficient nonbleeders and increased in FXI-deficient patients with prothrombotic phenotype. Receiver operating characteristic analysis indicated that TF-independent parameters were useful for discriminating FXI-deficient bleeders from non-bleeders. In FXI-deficient plasma spiked with FXI concentrate and in patients receiving FXI replacement, TD parameters were shifted toward hypercoagulation already at plasma FXI levels around 20%.

Conclusion: TF-independent coagulation parameters assessed by TD have the potential to identify the clinical phenotype in FXI-deficient patients and to monitor FXI replacement therapy.

MeSH terms

Blood Coagulation* / drug effects
Factor XI / therapeutic use*
Factor XI Deficiency / blood*
Factor XI Deficiency / diagnosis
Hemorrhage / blood
Hemorrhage / diagnosis
Humans
Prognosis
Thrombin / analysis
Thromboplastin / analysis*

Substances

Factor XI
Thromboplastin
Thrombin

Grants and funding

Takeda company/# IIR-CHE-001695