Factor XIa-specific IgG and a reversal agent to probe factor XI function in thrombosis and hemostasis

Thrombosis is a major cause of morbidity and mortality. Current antithrombotic drugs are not ideal in that they must balance prevention of thrombosis against bleeding risk. Inhibition of coagulation factor XI (FXI) may offer an improvement over existing antithrombotic strategies by preventing some f...

Full description

Saved in:
Bibliographic Details
Published inScience translational medicine Vol. 8; no. 353; p. 353ra112
Main Authors David, Tovo, Kim, Yun Cheol, Ely, Lauren K, Rondon, Isaac, Gao, Huilan, O'Brien, Peter, Bolt, Michael W, Coyle, Anthony J, Garcia, Jorge L, Flounders, Eric A, Mikita, Thomas, Coughlin, Shaun R
Format Journal Article
LanguageEnglish
Published United States 24.08.2016
Subjects
Animals
Antibodies, Blocking - metabolism
Antibodies, Monoclonal - metabolism
Antibody Specificity
Factor XI - physiology
Factor XIa - antagonists & inhibitors
Factor XIa - immunology
Hemostasis - physiology
Humans
Immunoglobulin G - metabolism
In Vitro Techniques
Kinetics
Macaca fascicularis
Mice
Rabbits
Thrombosis - blood
Online AccessGet more information

Cover

More Information
Summary:Thrombosis is a major cause of morbidity and mortality. Current antithrombotic drugs are not ideal in that they must balance prevention of thrombosis against bleeding risk. Inhibition of coagulation factor XI (FXI) may offer an improvement over existing antithrombotic strategies by preventing some forms of thrombosis with lower bleeding risk. To permit exploration of this hypothesis in humans, we generated and characterized a series of human immunoglobulin Gs (IgGs) that blocked FXIa active-site function but did not bind FXI zymogen or other coagulation proteases. The most potent of these IgGs, C24 and DEF, inhibited clotting in whole human blood and prevented FeCl3-induced carotid artery occlusion in FXI-deficient mice reconstituted with human FXI and in thread-induced venous thrombosis in rabbits at clinically relevant doses. At doses substantially higher than those required for inhibition of intravascular thrombus formation in these models, DEF did not increase cuticle bleeding in rabbits or cause spontaneous bleeding in macaques over a 2-week study. Anticipating the desirability of a reversal agent, we also generated a human IgG that rapidly reversed DEF activity ex vivo in human plasma and in vivo in rabbits. Thus, an active site-directed FXIa-specific antibody can block thrombosis in animal models and, together with the reversal agent, may facilitate exploration of the roles of FXIa in human disease.
ISSN:1946-6242
DOI:10.1126/scitranslmed.aaf4331