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The endothelial cell protein C receptor: cell surface conductor of cytoprotective coagulation factor signaling
被引:0
|作者:
Eimear M. Gleeson
James S. O’Donnell
Roger J. S. Preston
机构:
[1] St James Hospital Campus,Haemostasis Research Group, Department of Haematology, Institute of Molecular Medicine
[2] Trinity College Dublin,undefined
来源:
Cellular and Molecular Life Sciences
|
2012年
/
69卷
关键词:
Endothelial cell protein C receptor;
Coagulation proteases;
Protein C;
Factor VII;
Sepsis;
D O I:
暂无
中图分类号:
学科分类号:
摘要:
Increasing evidence links blood coagulation proteins with the regulation of acute and chronic inflammatory disease. Of particular interest are vitamin K-dependent proteases, which are generated as a hemostatic response to vascular injury, but can also initiate signal transduction via interactions with vascular receptors. The endothelial cell protein C receptor (EPCR) is a multi-ligand vitamin K-dependent protein receptor for zymogen and activated forms of plasma protein C and factor VII. Although the physiological role of the EPCR-FVII(a) interaction is not well-understood, protein C binding to EPCR facilitates rapid generation of APC in response to excessive thrombin generation, and is a central requirement for the multiple signal-transduction cascades initiated by APC on both vascular endothelial and innate immune cells. Exciting recent studies have highlighted the emerging role of EPCR in modulating the cytoprotective properties of APC in a number of diverse inflammatory disorders. In this review, we describe the structure–function relationships, signal transduction pathways, and cellular interactions that enable EPCR to modulate the anticoagulant and anti-inflammatory properties of its vitamin K-dependent protein ligands, and examine the relevance of EPCR to both thrombotic and inflammation-associated disease.
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页码:717 / 726
页数:9
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