Abstract

Cell activation by thrombin is critical for hemostasis and thrombosis, and may be important in inflammatory and proliferative responses in blood vessels. The goal of these studies is to determine the molecular mechanisms by which thrombin activates platelets and other cells. Thrombin activates cells by interacting with a specific cell surface molecule, the thrombin """"""""receptor"""""""". The thrombin receptor has not been identified. Moreover, whether thrombin activates its receptor by a novel proteolytic mechanism or by classical ligand binding is unknown. This basic information is critical for an understanding of thrombin signalling and for the rational design of thrombin inhibitors.
The specific aims of this proposal are: 1) to develop novel recombinant thrombins for use as reagents to define the role of thrombin's protease activity in thrombin-induced cell and platelet activation, and as ligands for affinity purification of the thrombin receptor, The role of thrombin's protease activity will be examined by using recombinant thrombins containing amino acid substitutions designed to abolish catalytic activity without perturbing substrate binding. The ability of these mutants to activate cells and platelets or to block activation by wild type thrombin will be determined. The goal of these studies is to develop not only thrombin receptor agonists or 'antagonists, but also novel affinity reagents for purifying the thrombin receptor. 2) to characterize and obtain a cDNA clone for the thrombin Two complementary approaches will be pursued to clone the thrombin receptor. (a) An assay for the mRNA encoding the thrombin receptor has been established using mRNA expression in xenopus oocytes. Both established and novel screening strategies will utilize this assay to obtain the thrombin receptor cDNA. (b) Recombinant thrombins which are proteolytically inactive yet retain receptor binding properties will be used as affinity agents to purify the thrombin receptor. With the thrombin receptor cDNA in hand we will address the following questions: Is the thrombin receptor cleaved by thrombin, and how does cleavage relate to activation? Do other thrombin receptor-like molecules exist and define a family of protease receptors? Which structural domains in thrombin and its receptor mediate binding? and What are the signal transduction molecules to which the receptor is coupled?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL044907-04
Application #
2221754
Study Section
Hematology Subcommittee 2 (HEM)
Project Start
1991-04-01
Project End
1995-04-30
Budget Start
1994-04-01
Budget End
1995-04-30
Support Year
4
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Bynagari-Settipalli, Yamini S; Cornelissen, Ivo; Palmer, Daniel et al. (2014) Redundancy and interaction of thrombin- and collagen-mediated platelet activation in tail bleeding and carotid thrombosis in mice. Arterioscler Thromb Vasc Biol 34:2563-9
Zhang, Cheng; Srinivasan, Yoga; Arlow, Daniel H et al. (2012) High-resolution crystal structure of human protease-activated receptor 1. Nature 492:387-92
Green, Jesse A; Suzuki, Kazuhiro; Cho, Bryan et al. (2011) The sphingosine 1-phosphate receptor S1P? maintains the homeostasis of germinal center B cells and promotes niche confinement. Nat Immunol 12:672-80
Shao, Bojing; Wahrenbrock, Mark G; Yao, Longbiao et al. (2011) Carcinoma mucins trigger reciprocal activation of platelets and neutrophils in a murine model of Trousseau syndrome. Blood 118:4015-23
Cornelissen, Ivo; Palmer, Daniel; David, Tovo et al. (2010) Roles and interactions among protease-activated receptors and P2ry12 in hemostasis and thrombosis. Proc Natl Acad Sci U S A 107:18605-10
Camerer, Eric; Barker, Adrian; Duong, Daniel N et al. (2010) Local protease signaling contributes to neural tube closure in the mouse embryo. Dev Cell 18:25-38
Hamilton, J R; Cornelissen, I; Mountford, J K et al. (2009) Atherosclerosis proceeds independently of thrombin-induced platelet activation in ApoE-/- mice. Atherosclerosis 205:427-32
Regard, Jean B; Sato, Isaac T; Coughlin, Shaun R (2008) Anatomical profiling of G protein-coupled receptor expression. Cell 135:561-71
Sood, Rashmi; Sholl, Lynette; Isermann, Berend et al. (2008) Maternal Par4 and platelets contribute to defective placenta formation in mouse embryos lacking thrombomodulin. Blood 112:585-91
Sood, Rashmi; Zogg, Mark; Westrick, Randal J et al. (2007) Fetal gene defects precipitate platelet-mediated pregnancy failure in factor V Leiden mothers. J Exp Med 204:1049-56

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