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Murine tissue factor disulfide mutation causes a bleeding phenotype with sex specific organ pathology and lethality

Authors :
Wolfram Ruf
Johannes Beckers
Marion Horsch
Felix C. Tanner
Tanja Klein-Rodewald
Thomas F. Lüscher
Andrea S. Rothmeier
Frauke Neff
Birgit Rathkolb
Martin Hrabě de Angelis
Simon F. Stämpfli
Anja Schrewe
Helmut Fuchs
Susanna H. M. Sluka
Alexander Akhmedov
Paula Grest
Valerie Gailus-Durner
Adrián Sanz-Moreno
Giovanni G. Camici
Eckhard Wolf
University of Zurich
Source :
Haematologica, Haematologica 105, 2484-2495 (2019)
Publication Year :
2019

Abstract

Tissue factor is highly expressed in sub-endothelial tissue. The extracellular allosteric disulfide bond Cys186-Cys209 of human tissue factor shows high evolutionary conservation and in vitro evidence suggests that it significantly contributes to tissue factor procoagulant activity. To investigate the role of this allosteric disulfide bond in vivo, we generated a C213G mutant tissue factor mouse by replacing Cys213 of the corresponding disulfide Cys190-Cys213 in murine tissue factor. A bleeding phenotype was prominent in homozygous C213G tissue factor mice. Pre-natal lethality of 1/3rd of homozygous offspring was observed between E9.5 and E14.5 associated with placental hemorrhages. After birth, homozygous mice suffered from bleedings in different organs and reduced survival. Homozygous C213G tissue factor male mice showed higher incidence of lung bleedings and lower survival rates than females. In both sexes, C213G mutation evoked a reduced protein expression (about 10-fold) and severely reduced pro-coagulant activity (about 1000-fold). Protein glycosylation was impaired and cell membrane exposure decreased in macrophages in vivo. Single housing of homozygous C213G tissue factor males reduced the occurrence of severe bleeding and significantly improved survival, suggesting that inter-male aggressiveness might significantly account for the sex differences. These experiments show that the tissue factor allosteric disulfide bond is of crucial importance for normal in vivo expression, post-translational processing and activity of murine tissue factor. Although C213G tissue factor mice do not display the severe embryonic lethality of tissue factor knock-out mice, their postnatal bleeding phenotype emphasizes the importance of fully functional tissue factor for hemostasis.

Details

ISSN :
15928721
Volume :
105
Issue :
10
Database :
OpenAIRE
Journal :
Haematologica
Accession number :
edsair.doi.dedup.....6d62206c901495c434a28961bc17b765