Abstract

Our laboratory has discovered the Nat-dependent allosteric enhancement of catalytic activity in thrombin and related serine proteases involved in blood coagulation and the complement system, identified the Na+ binding site and elucidated the importance of Na+ binding in the function and evolution of serine proteases. The proposed research project is aimed at gaining a detailed understanding of how Na+ is recognized by thrombin and how Na+ binding allosterically influences the structural determinants of activity and specificity of the enzyme. We will use a combination of kinetic and site-directed mutagenesis studies to dissect the structural determinants of the monovalent cation specificity of thrombin and to identify thrombin residues that are under the influence of Na+ binding and control recognition of physiologic substrates within the active site. Residues specifically involved in the binding and catalysis of fibrinogen, protein C and the thrombin receptors will be identified, thereby enabling a complete molecular dissection of thrombin multiple functions in the blood. We will also exploit the knowledge gained from the proposed research project on thrombin to rationally engineering Na+ binding and enhanced catalytic activity in the fibrinolytic enzyme tissue plasminogen activator. These studies will produce more proficient derivatives of the enzyme that may benefit the current treatment of acute myocardial infarction and stroke. Developments from the proposed research plan will broaden our understanding of the molecular aspects of thrombin function and regulation, will impact on the treatment and prevention of thrombotic disorders in which thrombin is directly involved, and will carry over to the study of other proteases in the blood coagulation cascade. By defining the rules for Na+ specificity in thrombin, these studies will generate important new knowledge relevant to allosteric proteins and enzymes activated by monovalent cations in general. Finally, these studies will demonstrate that proteases with enhanced catalytic activity can be engineered rationally to benefit areas of medical and biotechnological importance.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL058141-07
Application #
6623567
Study Section
Hematology Subcommittee 2 (HEM)
Program Officer
Link, Rebecca P
Project Start
1997-04-01
Project End
2007-03-31
Budget Start
2003-04-01
Budget End
2004-03-31
Support Year
7
Fiscal Year
2003
Total Cost
$390,848
Indirect Cost

  Institution

Name
Washington University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Vicente, Cristina P; Weiler, Hartmut; Di Cera, Enrico et al. (2012) Thrombomodulin is required for the antithrombotic activity of thrombin mutant W215A/E217A in a mouse model of arterial thrombosis. Thromb Res 130:646-8
Niu, Weiling; Chen, Zhiwei; Gandhi, Prafull S et al. (2011) Crystallographic and kinetic evidence of allostery in a trypsin-like protease. Biochemistry 50:6301-7
Gohara, David W; Di Cera, Enrico (2011) Allostery in trypsin-like proteases suggests new therapeutic strategies. Trends Biotechnol 29:577-85
Pozzi, Nicola; Chen, Raymond; Chen, Zhiwei et al. (2011) Rigidification of the autolysis loop enhances Na(+) binding to thrombin. Biophys Chem 159:6-13
Di Cera, Enrico (2011) Thrombin as an anticoagulant. Prog Mol Biol Transl Sci 99:145-84
Rana, Sadhna; Pozzi, Nicola; Pelc, Leslie A et al. (2011) Redesigning allosteric activation in an enzyme. Proc Natl Acad Sci U S A 108:5221-5
Pozzi, Nicola; Chen, Zhiwei; Zapata, Fatima et al. (2011) Crystal structures of prethrombin-2 reveal alternative conformations under identical solution conditions and the mechanism of zymogen activation. Biochemistry 50:10195-202
Berny-Lang, Michelle A; Hurst, Sawan; Tucker, Erik I et al. (2011) Thrombin mutant W215A/E217A treatment improves neurological outcome and reduces cerebral infarct size in a mouse model of ischemic stroke. Stroke 42:1736-41
Gandhi, Prafull S; Chen, Zhiwei; Appelbaum, Eric et al. (2011) Structural basis of thrombin-protease-activated receptor interactions. IUBMB Life 63:375-82
Flick, Matthew J; Chauhan, Anil K; Frederick, Malinda et al. (2011) The development of inflammatory joint disease is attenuated in mice expressing the anticoagulant prothrombin mutant W215A/E217A. Blood 117:6326-37

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