The role of tissue factor/factor VIIa in the pathophysiology of acute thrombotic formation

Thomas J. Girard; Nancy S. Nicholson

doi:10.1016/S1471-4892(01)00031-5

The role of tissue factor/factor VIIa in the pathophysiology of acute thrombotic formation

Thomas J. Girard, Nancy S. Nicholson

Department of Pediatrics

Research output: Contribution to journal › Review article › peer-review

39 Scopus citations

Abstract

Tissue factor (TF) is the essential cofactor for the coagulation protease factor VIIa (FVIIa), initiating the coagulation cascade. The role of TF in thrombotic diseases is becoming increasingly evident. Recent findings suggest that inhibition of TF/FVIIa activity could be important in the prevention of clinical sequelae associated with plaque rupture or vessel damage that exposes TF to blood. Furthermore, selective inhibitors of TF/FVIIa may be associated with less bleeding risk than other antithrombotic agents. Several TF/FVIIa inhibitors are in development, including the protein-based inhibitors (such as NAPc2, Corsevin M™, FFR-FVIIa, and Tifacogin). Research into the development of small molecule inhibitors is on-going, but is at a less advanced stage.

Original language	English
Pages (from-to)	159-163
Number of pages	5
Journal	Current Opinion in Pharmacology
Volume	1
Issue number	2
DOIs	https://doi.org/10.1016/S1471-4892(01)00031-5
State	Published - Apr 1 2001

Keywords

Acute coronary syndromes
Drug Discovery
Heparin
Hirudin
Molecular Medicine
Myocardial infarction
Pharmacology
TF/FVIIa
Thrombosis
Tick anticoagulant protein
Tissue factor

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10.1016/S1471-4892(01)00031-5

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title = "The role of tissue factor/factor VIIa in the pathophysiology of acute thrombotic formation",

abstract = "Tissue factor (TF) is the essential cofactor for the coagulation protease factor VIIa (FVIIa), initiating the coagulation cascade. The role of TF in thrombotic diseases is becoming increasingly evident. Recent findings suggest that inhibition of TF/FVIIa activity could be important in the prevention of clinical sequelae associated with plaque rupture or vessel damage that exposes TF to blood. Furthermore, selective inhibitors of TF/FVIIa may be associated with less bleeding risk than other antithrombotic agents. Several TF/FVIIa inhibitors are in development, including the protein-based inhibitors (such as NAPc2, Corsevin M{\texttrademark}, FFR-FVIIa, and Tifacogin). Research into the development of small molecule inhibitors is on-going, but is at a less advanced stage.",

keywords = "Acute coronary syndromes, Drug Discovery, Heparin, Hirudin, Molecular Medicine, Myocardial infarction, Pharmacology, TF/FVIIa, Thrombosis, Tick anticoagulant protein, Tissue factor",

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AU - Girard, Thomas J.

AU - Nicholson, Nancy S.

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N2 - Tissue factor (TF) is the essential cofactor for the coagulation protease factor VIIa (FVIIa), initiating the coagulation cascade. The role of TF in thrombotic diseases is becoming increasingly evident. Recent findings suggest that inhibition of TF/FVIIa activity could be important in the prevention of clinical sequelae associated with plaque rupture or vessel damage that exposes TF to blood. Furthermore, selective inhibitors of TF/FVIIa may be associated with less bleeding risk than other antithrombotic agents. Several TF/FVIIa inhibitors are in development, including the protein-based inhibitors (such as NAPc2, Corsevin M™, FFR-FVIIa, and Tifacogin). Research into the development of small molecule inhibitors is on-going, but is at a less advanced stage.

AB - Tissue factor (TF) is the essential cofactor for the coagulation protease factor VIIa (FVIIa), initiating the coagulation cascade. The role of TF in thrombotic diseases is becoming increasingly evident. Recent findings suggest that inhibition of TF/FVIIa activity could be important in the prevention of clinical sequelae associated with plaque rupture or vessel damage that exposes TF to blood. Furthermore, selective inhibitors of TF/FVIIa may be associated with less bleeding risk than other antithrombotic agents. Several TF/FVIIa inhibitors are in development, including the protein-based inhibitors (such as NAPc2, Corsevin M™, FFR-FVIIa, and Tifacogin). Research into the development of small molecule inhibitors is on-going, but is at a less advanced stage.

KW - Acute coronary syndromes

KW - Drug Discovery

KW - Heparin

KW - Hirudin

KW - Molecular Medicine

KW - Myocardial infarction

KW - Pharmacology

KW - TF/FVIIa

KW - Thrombosis

KW - Tick anticoagulant protein

KW - Tissue factor

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AN - SCOPUS:0035321911

SN - 1471-4892

VL - 1

SP - 159

EP - 163

JO - Current Opinion in Pharmacology

JF - Current Opinion in Pharmacology

IS - 2

ER -

The role of tissue factor/factor VIIa in the pathophysiology of acute thrombotic formation

Abstract

Keywords

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