Abstract

Activation of the blood plasma (a cellular) coagulation cascade by contact with materials is thought to be initiated by molecular assembly of the proteins of the activation complex directly onto procoagulant surfaces, leading to conversion of the zymogen Factor XII to the protease form FXIIa that desorbs into the solution phase. This mechanism is at odds with the experimental observation that the efficiency of contact activation is critically dependant on procoagulant surface energy in reverse order of protein adsorbent capacity, with very efficient activation for high-surface energy (water wettable) surfaces that are inefficient protein adsorbents and inefficient activation for intermediate- and low-energy (poorly water wettable) surfaces that are efficient adsorbents. Furthermore, it is difficult to rationalize from a surface energetic perspective how procoagulant surfaces can simultaneously serve as efficient FXII adsorbents (leading to molecular assembly on a surface) and inefficient FXIIa adsorbents (leading to release from a surface), especially in view of the relatively minor molecular difference between zymogen and protease forms. These and other discrepancies between proposed mechanism and experiment can be rationalized by an alternative hypothesis proposing that: Proteins of the contact activation complex assemble near procoagulant surfaces within a vicinal water region having special solvent properties that result from the hydration of high-energy surfaces. Self-amplifying zymogen-enzyme conversion occurs within this vicinal water zone, but not directly on surfaces, and propagates into the bulk plasma phase therefrom. Solvent properties of water near intermediate-to-low surface energy materials does not induce activation of FXII and adsorption directly onto these relatively hydrophobic surfaces does not potentiate the intrinsic pathway of the plasma coagulation cascade. The overarching objective of the work outlined within this application is to test the veracity of this proposition and underlying lemma with an eye to elucidating surface-engineering routes to materials with improved hemocompatibility for blood- contact applications. The proposed work is a balanced mix of biophysical and hematological approaches to a long-standing bioengineering problem that will relate surface thermodynamics of protein adsorption, surface-protein binding directly measured by AFM, and the procoagulant efficiency of surfaces variably bearing immobilized factors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL069965-01
Application #
6463492
Study Section
Surgery and Bioengineering Study Section (SB)
Program Officer
Link, Rebecca P
Project Start
2002-04-01
Project End
2006-03-31
Budget Start
2002-04-01
Budget End
2003-03-31
Support Year
1
Fiscal Year
2002
Total Cost
$307,800
Indirect Cost

  Institution

Name
Pennsylvania State University
Department
Surgery
Type
Schools of Medicine
DUNS #
129348186
City
Hershey
State
PA
Country
United States
Zip Code
17033

  Publications

Xu, Li-Chong; Wo, Yaqi; Meyerhoff, Mark E et al. (2017) Inhibition of bacterial adhesion and biofilm formation by dual functional textured and nitric oxide releasing surfaces. Acta Biomater 51:53-65
Bauer, James W; Xu, Li-Chong; Vogler, Erwin A et al. (2017) Surface dependent contact activation of factor XII and blood plasma coagulation induced by mixed thiol surfaces. Biointerphases 12:02D410
Golas, Avantika; Pitakjakpipop, Harit; Rahn, Matthew S et al. (2015) Enzymes produced by autoactivation of blood factor XII in buffer: A contribution from the Hematology at Biomaterial Interfaces Research Group. Biomaterials 37:1-12
Xu, Li-Chong; Bauer, James W; Siedlecki, Christopher A (2014) Proteins, platelets, and blood coagulation at biomaterial interfaces. Colloids Surf B Biointerfaces 124:49-68
Krishnan, Anandi; Vogler, Erwin A; Sullenger, Bruce A et al. (2013) The effect of surface contact activation and temperature on plasma coagulation with an RNA aptamer directed against factor IXa. J Thromb Thrombolysis 35:48-56
Noh, Hyeran; Barnthip, Naris; Parhi, Purnendu et al. (2013) Electrophoretic implementation of the solution-depletion method for measuring protein adsorption, adsorption kinetics, and adsorption competition among multiple proteins in solution. Methods Mol Biol 1025:157-66
Golas, Avantika; Yeh, Chyi-Huey Josh; Pitakjakpipop, Harit et al. (2013) A comparison of blood factor XII autoactivation in buffer, protein cocktail, serum, and plasma solutions. Biomaterials 34:607-20
Josh Yeh, Chyi-Huey; Dimachkie, Ziad O; Golas, Avantika et al. (2012) Contact activation of blood plasma and factor XII by ion-exchange resins. Biomaterials 33:9-19
Vogler, Erwin A (2012) Protein adsorption in three dimensions. Biomaterials 33:1201-37
Vogler, Erwin A (2011) The Goldilocks surface. Biomaterials 32:6670-5

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