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Combined factor VII/protein C deficiency results in intrauterine coagulopathy in mice
Joyce C.Y. Chan, Ivo Cornelissen, Desire Collen, Victoria A. Ploplis, Francis J. Castellino
Joyce C.Y. Chan, Ivo Cornelissen, Desire Collen, Victoria A. Ploplis, Francis J. Castellino
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Combined factor VII/protein C deficiency results in intrauterine coagulopathy in mice

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Abstract

To determine whether an additional loss of the coagulation factor VII (FVII) gene influenced the coagulopathy observed in protein C gene–deficient (PC–/–) embryos and neonates, we crossed mice doubly heterozygous for the factor VII (FVII+/–) and protein C (PC+/–) genes to produce offspring possessing the 9 predicted genotypic combinations. FVII–/–/PC–/– embryos, although present at their expected Mendelian frequency, displayed a phenotype that had not been observed in either the FVII or PC singly deficient embryos. At E12.5 days postcoitum (dpc), FVII–/–/PC–/– embryos demonstrated an intra- and extravascular coagulopathy that progressed with substantial concomitant hemorrhage and peripheral edema by E17.5dpc, resulting in mortality immediately after birth. FVII+/–/PC–/– embryos showed a less severe phenotype, suggesting a gene dosage effect. The lack of rescue of PC–/– embryos and neonates and augmented coagulopathy resulting from an additional heterozygous or homozygous FVII deficiency are probably due to increased factor Xa and thrombin generation, resulting from loss of FVIIa-dependent tissue factor pathway inhibitor function and the absence of control at the levels of factors Va and VIIIa. The presence of fibrin in embryos in the absence of fetal FVII suggests that significant clot-generating potential exists outside of the embryonic factor VII–dependent pathway.

Authors

Joyce C.Y. Chan, Ivo Cornelissen, Desire Collen, Victoria A. Ploplis, Francis J. Castellino

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Figure 1

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Analysis of an E17.5dpc FVII–/–/PC–/– embryo. (a) Gross appearance displ...
Analysis of an E17.5dpc FVII–/–/PC–/– embryo. (a) Gross appearance displaying significant internal and peripheral hemorrhage and edema. (b–c) H&E staining of liver sections indicating areas of fibrosis within 1 of the lobes (arrow) (b); anti-fibrinogen immunostaining of parallel liver sections demonstrating interstitial fibrin deposition (brown) around these fibrotic patches (c). (d–g) Histological analyses of hindbrain sections indicating areas of hemorrhage (d), fibrin deposition (e), collagen deposition (blue) (f), and the presence of CD45-positive leukocytes (brown) (g). (h–j) Histological analyses of atrial sections confirming the presence of blood in the atria (h), fibrin deposition (i), and internal collagen invasion around these areas of fibrin (j).

Copyright © 2025 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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