Protein C is an important regulatory mechanism of blood coagulation. Protein C functions as an anticoagulant when converted to the active serine protease form on the endothelial cell surface. Thrombomodulin (TM), an endothelial cell surface receptor specific for thrombin, has been identified as an essential component for protein C activation. Although protein C can be activated directly by the thrombin–TM complex, the conversion is known as a relatively low-affinity reaction. Therefore, protein C activation has been believed to occur only in microcirculation. On the other hand, we have identified and cloned a novel endothelial cell surface receptor (EPCR) that is capable of high-affinity binding of protein C and activated protein C. In this study, we demonstrate the constitutive, endothelial cell–specific expression of EPCR in vivo. Abundant expression was particularly detected in the aorta and large arteries. In vitro cultured, arterial endothelial cells were also found to express abundant EPCR and were capable of promoting significant levels of protein C activation. EPCR was found to greatly accelerate protein C activation by examining functional activity in transfected cell lines expressing EPCR and/or TM. EPCR decreased the dissociation constant and increased the maximum velocity for protein C activation mediated by the thrombin–TM complex. By these mechanisms, EPCR appears to enable significant levels of protein C activation in large vessels. These results suggest that the protein C anticoagulation pathway is important for the regulation of blood coagulation not only in microvessels but also in large vessels.
Skip Nav Destination
Article navigation
6 April 1998
Article|
April 06 1998
Activation Mechanism of Anticoagulant Protein C in Large Blood Vessels Involving the Endothelial Cell Protein C Receptor
Kenji Fukudome,
Kenji Fukudome
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Xiaofen Ye,
Xiaofen Ye
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Naoko Tsuneyoshi,
Naoko Tsuneyoshi
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Osamu Tokunaga,
Osamu Tokunaga
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Keishin Sugawara,
Keishin Sugawara
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Hiroshi Mizokami,
Hiroshi Mizokami
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Masao Kimoto
Masao Kimoto
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Search for other works by this author on:
Kenji Fukudome
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Xiaofen Ye
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Naoko Tsuneyoshi
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Osamu Tokunaga
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Keishin Sugawara
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Hiroshi Mizokami
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Masao Kimoto
From the *Department of Immunology and the ‡Department of Pathology, Saga Medical School, Nabeshima, Saga 849, Japan; and the §Applied Research Laboratory, The Chemo-Sero-Therapeutic Research Institute, Shimizu, Kumamoto 860, Japan
Address correspondence to Kenji Fukudome, Department of Immunology, Saga Medical School, 5-1-1 Nabeshima, Saga 849, Japan. Phone: 81-952-34-2256; Fax: 81-952-34-2049; E-mail: [email protected]
1Abbreviations used in this paper: AEC, arterial endothelial cell; APC, activated protein C; EPCR, endothelial cell protein C-APC receptor; TM, thrombomodulin; VEC, venous endothelial cell.
Received:
October 28 1996
Revision Received:
December 15 1997
Online ISSN: 1540-9538
Print ISSN: 0022-1007
1998
J Exp Med (1998) 187 (7): 1029–1035.
Article history
Received:
October 28 1996
Revision Received:
December 15 1997
Citation
Kenji Fukudome, Xiaofen Ye, Naoko Tsuneyoshi, Osamu Tokunaga, Keishin Sugawara, Hiroshi Mizokami, Masao Kimoto; Activation Mechanism of Anticoagulant Protein C in Large Blood Vessels Involving the Endothelial Cell Protein C Receptor . J Exp Med 6 April 1998; 187 (7): 1029–1035. doi: https://doi.org/10.1084/jem.187.7.1029
Download citation file:
Sign in
Don't already have an account? Register
Client Account
You could not be signed in. Please check your email address / username and password and try again.
Could not validate captcha. Please try again.
Sign in via your Institution
Sign in via your InstitutionSuggested Content
Email alerts
Advertisement