Cause-effect relation between hyperfibrinogenemia and vascular disease

Thrombin exosite 1 binds the predominant ␥ A /␥ A -fibrin form with low affinity. A subpopulation of fibrin molecules, ␥ A /␥-fibrin, has an extended COOH terminus ␥-chain that binds exosite 2 of thrombin. Bivalent binding to ␥ A /␥-fibrin increases the affinity of thrombin 10-fold, as determined by surface plasmon resonance. Because of its higher affinity, thrombin dissociates 7-fold more slowly from ␥ A /␥-fibrin clots than from ␥ A /␥ A -fibrin clots. After 24 h of washing, however, both ␥ A /␥-and ␥ A /␥ A -fibrin clots generate fibrinopeptide A when incubated with fibrinogen, indicating the retention of active thrombin. Previous studies demonstrated that heparin heightens the affinity of thrombin for fibrin by simultaneously binding to fibrin and exosite 2 on thrombin to generate a ternary heparinthrombin-fibrin complex that protects thrombin from inhibition by antithrombin and heparin cofactor II. In contrast, dermatan sulfate does not promote ternary complex formation because it does not bind to fibrin. Heparin-catalyzed rates of thrombin inhibition by antithrombin were 5-fold slower in ␥ A /␥-fibrin clots than they were in ␥ A /␥ A -fibrin clots. This difference reflects bivalent binding of thrombin to ␥ A /␥-fibrin because (a) it is abolished by addition of a ␥-chaindirected antibody that blocks exosite 2-mediated binding of thrombin to the ␥-chain and (b) the dermatan sulfate-catalyzed rate of thrombin inhibition by heparin cofactor II also is lower with ␥ A /␥-fibrin than with ␥ A /␥ A -fibrin clots. Thus, bivalent binding of thrombin to ␥ A /␥-fibrin protects thrombin from inhibition, raising the possibility that ␥ A /␥-fibrin serves as a reservoir of active thrombin that renders thrombi thrombogenic.

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“…Taken together, these findings support the concept that fibrin-bound thrombin contributes to the thrombogenic potential of thrombi (27,37).…”

Section: Discussionsupporting

confidence: 75%

Bivalent Binding to γA/γ′-Fibrin Engages Both Exosites of Thrombin and Protects It from Inhibition by the Antithrombin-Heparin Complex

Fredenburgh

Stafford

Leslie

et al. 2008

Journal of Biological Chemistry

109

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“…By stabilizing intravascular fibrin, which often forms in response to vascular injury and which can be invaded by VSMCs and other cell types to form a neointima, PAI-1 may promote intimal hyperplasia. 7 Consistent with this hypothesis, hyperfibrinogenemic mice exhibit enhanced neointima formation after carotid artery ligation compared with wild-type mice, 50 and depletion of plasma fibrinogen by administration of ancrod reduces intimal hyperplasia in mice after carotid artery ligation. 51 However, ␣ 2 -antiplasmin deficiency, which promotes fibrinolysis in vivo, 32 has no effect on neointima formation in mice, 52 suggesting that stabilization of fibrin by PAI-1 and/or ␣ 2 -antiplasmin does not play an essential role in murine vascular remodeling.…”

Section: Role Of Pa System In Controlling Intimal Hyperplasia After Vsupporting

confidence: 55%

Vascular Functions of the Plasminogen Activation System

Fay

Garg

Sunkar

2007

ATVB

122

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Abstract-The plasminogen activator (PA) system, which controls the formation and activity of plasmin, plays a key role in modulating hemostasis, thrombosis, and several other biological processes. While a great deal is known about the function of the PA system, it remains a focus of intensive investigation, and the list of biological pathways and human diseases that are modulated by normal and pathologic function of its components continues to lengthen. Because of remarkable advances in molecular genetics, the laboratory mouse has become the most useful animal system to study the normal and pathologic functions of the PA system. The purpose of this review is to summarize studies that have used genetically modified mice to examine the functions of the PA system in hemostasis and thrombosis, intimal hyperplasia after vascular injury, and atherosclerosis. Particular emphasis is placed on the vascular functions of PA inhibitor-1, a key regulator of the PA system, and the multiple variables that appear to account for the complex role of PA inhibitor-1 in regulating vascular remodeling. Lastly, the strengths and limitations of using mice to model human vascular disease processes are discussed. (Arterioscler Thromb Vasc Biol.

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“…9,28 In addition to its role as an inflammatory biomarker, fibrinogen is the predominant coagulation factor in blood plasma and plays an important role in platelet aggregation, fibrin formation, and plasma visosity. 29,30 Our findings suggest that plasma fibrinogen levels may reflect both an inflammatory and a prothrombotic state because the risk associated with higher fibrinogen levels was only partially accounted for by higher hs-CRP levels. Attenuation of the risk associated with fibrinogen after adjustment for hs-CRP, and vice versa, may be explained by potential confounding, or possible mediation, of some of the effect of fibrinogen via inflammation.…”

Section: Discussionmentioning

confidence: 83%

Additive Value of Immunoassay-Measured Fibrinogen and High-Sensitivity C-Reactive Protein Levels for Predicting Incident Cardiovascular Events

et al. 2006

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Background-Current guidelines suggest measuring high-sensitivity C-reactive protein (hs-CRP) as an aid to coronary risk assessment in adults without cardiovascular disease (CVD). Whether other inflammatory biomarkers, such as fibrinogen, add further prognostic information is uncertain. Methods and Results-In a prospective study of 27 742 initially healthy middle-aged women, the associations of baseline immunoassay fibrinogen and hs-CRP measurements with incident CVD were examined over a 10-year follow-up period.

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Cause-effect relation between hyperfibrinogenemia and vascular disease

Cited by 78 publications

References 52 publications

Bivalent Binding to γA/γ′-Fibrin Engages Both Exosites of Thrombin and Protects It from Inhibition by the Antithrombin-Heparin Complex

Bivalent Binding to γA/γ′-Fibrin Engages Both Exosites of Thrombin and Protects It from Inhibition by the Antithrombin-Heparin Complex

Vascular Functions of the Plasminogen Activation System

Additive Value of Immunoassay-Measured Fibrinogen and High-Sensitivity C-Reactive Protein Levels for Predicting Incident Cardiovascular Events

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