Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation

Woosuk S. Hur; David S. Paul; Emma G. Bouck; Oscar A. Negrón; Jean Marie Mwiza; Lauren G. Poole; Holly M. Cline-Fedewa; Emily G. Clark; Lih Jiin Juang; Jerry Leung; Christian J. Kastrup; Tatiana P. Ugarova; Alisa S. Wolberg; James P. Luyendyk; Wolfgang Bergmeier; Matthew J. Flick

doi:10.1182/blood.2021012537

Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation

Woosuk S. Hur
, David S. Paul
, Emma G. Bouck
, Oscar A. Negrón
, Jean Marie Mwiza
, Lauren G. Poole
, Holly M. Cline-Fedewa
, Emily G. Clark
, Lih Jiin Juang
, Jerry Leung
, Christian J. Kastrup
, Tatiana P. Ugarova
, Alisa S. Wolberg
, James P. Luyendyk
, Wolfgang Bergmeier
, Matthew J. Flick

Physician Assistant Studies

Research output: Contribution to journal › Article › peer-review

24 Scopus citations

Abstract

Genetic variants within the fibrinogen Aα chain encoding the αC-region commonly result in hypodysfibrinogenemia in patients. However, the (patho)physiological consequences and underlying mechanisms of such mutations remain undefined. Here, we generated Fga270 mice carrying a premature termination codon within the Fga gene at residue 271. The Fga270 mutation was compatible with Mendelian inheritance for offspring of heterozygous crosses. Adult Fga270/270 mice were hypofibrinogenemic with ∼10% plasma fibrinogen levels relative to FgaWT/WT mice, linked to 90% reduction in hepatic Fga messenger RNA (mRNA) because of nonsense-mediated decay of the mutant mRNA. Fga270/270 mice had preserved hemostatic potential in vitro and in vivo in models of tail bleeding and laser-induced saphenous vein injury, whereas Fga−/− mice had continuous bleeding. Platelets from FgaWT/WT and Fga270/270 mice displayed comparable initial aggregation following adenosine 5′-diphosphate stimulation, but Fga270/270 platelets quickly disaggregated. Despite ∼10% plasma fibrinogen, the fibrinogen level in Fga270/270 platelets was ∼30% of FgaWT/WT platelets with a compensatory increase in fibronectin. Notably, Fga270/270 mice showed complete protection from thrombosis in the inferior vena cava stasis model. In a model of Staphylococcus aureus peritonitis, Fga270/270 mice supported local, fibrinogen-mediated bacterial clearance and host survival comparable to FgaWT/WT, unlike Fga−/− mice. Decreasing the normal fibrinogen levels to ∼10% with small interfering RNA in mice also provided significant protection from venous thrombosis without compromising hemostatic potential and antimicrobial function. These findings both reveal novel molecular mechanisms underpinning fibrinogen αC-region truncation mutations and highlight the concept that selective fibrinogen reduction may be efficacious for limiting thrombosis while preserving hemostatic and immune protective functions.

Original language	English
Pages (from-to)	1374-1388
Number of pages	15
Journal	Blood
Volume	139
Issue number	9
DOIs	https://doi.org/10.1182/blood.2021012537
State	Published - Mar 3 2022

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Hur, W. S., Paul, D. S., Bouck, E. G., Negrón, O. A., Mwiza, J. M., Poole, L. G., Cline-Fedewa, H. M., Clark, E. G., Juang, L. J., Leung, J., Kastrup, C. J., Ugarova, T. P., Wolberg, A. S., Luyendyk, J. P., Bergmeier, W., & Flick, M. J. (2022). Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation. Blood, 139(9), 1374-1388. https://doi.org/10.1182/blood.2021012537

@article{e889e290cdeb408784f729851595eadc,

title = "Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation",

abstract = "Genetic variants within the fibrinogen Aα chain encoding the αC-region commonly result in hypodysfibrinogenemia in patients. However, the (patho)physiological consequences and underlying mechanisms of such mutations remain undefined. Here, we generated Fga270 mice carrying a premature termination codon within the Fga gene at residue 271. The Fga270 mutation was compatible with Mendelian inheritance for offspring of heterozygous crosses. Adult Fga270/270 mice were hypofibrinogenemic with ∼10\% plasma fibrinogen levels relative to FgaWT/WT mice, linked to 90\% reduction in hepatic Fga messenger RNA (mRNA) because of nonsense-mediated decay of the mutant mRNA. Fga270/270 mice had preserved hemostatic potential in vitro and in vivo in models of tail bleeding and laser-induced saphenous vein injury, whereas Fga−/− mice had continuous bleeding. Platelets from FgaWT/WT and Fga270/270 mice displayed comparable initial aggregation following adenosine 5′-diphosphate stimulation, but Fga270/270 platelets quickly disaggregated. Despite ∼10\% plasma fibrinogen, the fibrinogen level in Fga270/270 platelets was ∼30\% of FgaWT/WT platelets with a compensatory increase in fibronectin. Notably, Fga270/270 mice showed complete protection from thrombosis in the inferior vena cava stasis model. In a model of Staphylococcus aureus peritonitis, Fga270/270 mice supported local, fibrinogen-mediated bacterial clearance and host survival comparable to FgaWT/WT, unlike Fga−/− mice. Decreasing the normal fibrinogen levels to ∼10\% with small interfering RNA in mice also provided significant protection from venous thrombosis without compromising hemostatic potential and antimicrobial function. These findings both reveal novel molecular mechanisms underpinning fibrinogen αC-region truncation mutations and highlight the concept that selective fibrinogen reduction may be efficacious for limiting thrombosis while preserving hemostatic and immune protective functions.",

author = "Hur, \{Woosuk S.\} and Paul, \{David S.\} and Bouck, \{Emma G.\} and Negr{\'o}n, \{Oscar A.\} and Mwiza, \{Jean Marie\} and Poole, \{Lauren G.\} and Cline-Fedewa, \{Holly M.\} and Clark, \{Emily G.\} and Juang, \{Lih Jiin\} and Jerry Leung and Kastrup, \{Christian J.\} and Ugarova, \{Tatiana P.\} and Wolberg, \{Alisa S.\} and Luyendyk, \{James P.\} and Wolfgang Bergmeier and Flick, \{Matthew J.\}",

year = "2022",

month = mar,

day = "3",

doi = "10.1182/blood.2021012537",

language = "English",

volume = "139",

pages = "1374--1388",

journal = "Blood",

issn = "0006-4971",

publisher = "Elsevier B.V.",

number = "9",

}

Hur, WS, Paul, DS, Bouck, EG, Negrón, OA, Mwiza, JM, Poole, LG, Cline-Fedewa, HM, Clark, EG, Juang, LJ, Leung, J, Kastrup, CJ, Ugarova, TP, Wolberg, AS, Luyendyk, JP, Bergmeier, W & Flick, MJ 2022, 'Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation', Blood, vol. 139, no. 9, pp. 1374-1388. https://doi.org/10.1182/blood.2021012537

TY - JOUR

T1 - Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation

AU - Hur, Woosuk S.

AU - Paul, David S.

AU - Bouck, Emma G.

AU - Negrón, Oscar A.

AU - Mwiza, Jean Marie

AU - Poole, Lauren G.

AU - Cline-Fedewa, Holly M.

AU - Clark, Emily G.

AU - Juang, Lih Jiin

AU - Leung, Jerry

AU - Kastrup, Christian J.

AU - Ugarova, Tatiana P.

AU - Wolberg, Alisa S.

AU - Luyendyk, James P.

AU - Bergmeier, Wolfgang

AU - Flick, Matthew J.

PY - 2022/3/3

Y1 - 2022/3/3

N2 - Genetic variants within the fibrinogen Aα chain encoding the αC-region commonly result in hypodysfibrinogenemia in patients. However, the (patho)physiological consequences and underlying mechanisms of such mutations remain undefined. Here, we generated Fga270 mice carrying a premature termination codon within the Fga gene at residue 271. The Fga270 mutation was compatible with Mendelian inheritance for offspring of heterozygous crosses. Adult Fga270/270 mice were hypofibrinogenemic with ∼10% plasma fibrinogen levels relative to FgaWT/WT mice, linked to 90% reduction in hepatic Fga messenger RNA (mRNA) because of nonsense-mediated decay of the mutant mRNA. Fga270/270 mice had preserved hemostatic potential in vitro and in vivo in models of tail bleeding and laser-induced saphenous vein injury, whereas Fga−/− mice had continuous bleeding. Platelets from FgaWT/WT and Fga270/270 mice displayed comparable initial aggregation following adenosine 5′-diphosphate stimulation, but Fga270/270 platelets quickly disaggregated. Despite ∼10% plasma fibrinogen, the fibrinogen level in Fga270/270 platelets was ∼30% of FgaWT/WT platelets with a compensatory increase in fibronectin. Notably, Fga270/270 mice showed complete protection from thrombosis in the inferior vena cava stasis model. In a model of Staphylococcus aureus peritonitis, Fga270/270 mice supported local, fibrinogen-mediated bacterial clearance and host survival comparable to FgaWT/WT, unlike Fga−/− mice. Decreasing the normal fibrinogen levels to ∼10% with small interfering RNA in mice also provided significant protection from venous thrombosis without compromising hemostatic potential and antimicrobial function. These findings both reveal novel molecular mechanisms underpinning fibrinogen αC-region truncation mutations and highlight the concept that selective fibrinogen reduction may be efficacious for limiting thrombosis while preserving hemostatic and immune protective functions.

AB - Genetic variants within the fibrinogen Aα chain encoding the αC-region commonly result in hypodysfibrinogenemia in patients. However, the (patho)physiological consequences and underlying mechanisms of such mutations remain undefined. Here, we generated Fga270 mice carrying a premature termination codon within the Fga gene at residue 271. The Fga270 mutation was compatible with Mendelian inheritance for offspring of heterozygous crosses. Adult Fga270/270 mice were hypofibrinogenemic with ∼10% plasma fibrinogen levels relative to FgaWT/WT mice, linked to 90% reduction in hepatic Fga messenger RNA (mRNA) because of nonsense-mediated decay of the mutant mRNA. Fga270/270 mice had preserved hemostatic potential in vitro and in vivo in models of tail bleeding and laser-induced saphenous vein injury, whereas Fga−/− mice had continuous bleeding. Platelets from FgaWT/WT and Fga270/270 mice displayed comparable initial aggregation following adenosine 5′-diphosphate stimulation, but Fga270/270 platelets quickly disaggregated. Despite ∼10% plasma fibrinogen, the fibrinogen level in Fga270/270 platelets was ∼30% of FgaWT/WT platelets with a compensatory increase in fibronectin. Notably, Fga270/270 mice showed complete protection from thrombosis in the inferior vena cava stasis model. In a model of Staphylococcus aureus peritonitis, Fga270/270 mice supported local, fibrinogen-mediated bacterial clearance and host survival comparable to FgaWT/WT, unlike Fga−/− mice. Decreasing the normal fibrinogen levels to ∼10% with small interfering RNA in mice also provided significant protection from venous thrombosis without compromising hemostatic potential and antimicrobial function. These findings both reveal novel molecular mechanisms underpinning fibrinogen αC-region truncation mutations and highlight the concept that selective fibrinogen reduction may be efficacious for limiting thrombosis while preserving hemostatic and immune protective functions.

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U2 - 10.1182/blood.2021012537

DO - 10.1182/blood.2021012537

M3 - Article

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SN - 0006-4971

VL - 139

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JO - Blood

JF - Blood

IS - 9

ER -

Hypofibrinogenemia with preserved hemostasis and protection from thrombosis in mice with an Fga truncation mutation

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