AI Article Synopsis

  • - The study tested ten types of specially made polyurethanes (PUs) to see how their surface properties influence platelet adhesion, focusing on factors like hydrophilicity and the adsorption of proteins like fibrinogen (Fg) and von Willebrand's factor (vWf).
  • - It was found that PUs that didn't absorb Fg showed very low platelet adhesion, indicating that Fg is crucial for this process; however, some hydrophobic PUs with high Fg absorption surprisingly displayed lower adhesion.
  • - The research also involved monoclonal antibodies that bind to specific parts of Fg, revealing that the binding to one specific site on Fg correlated strongly with platelet adhesion, while other sites could partially block adhesion,

Article Abstract

Ten specially synthesized polyurethanes (PUs) were used to investigate the effects of surface properties on platelet adhesion. Surface composition and hydrophilicity, fibrinogen (Fg) and von Willebrand's factor (vWf) adsorption, monoclonal anti-Fg binding, and platelet adhesion were measured. PUs preadsorbed with afibrinogenemic plasma or serum exhibited very low platelet adhesion, while adhesion after preadsorption with vWf deficient plasma was not reduced, showing that Fg is the key plasma protein mediating platelet adhesion under static conditions. Platelet adhesion to the ten PUs after plasma preadsorption varied greatly, but was only partially consistent with Fg adsorption. Thus, while very hydrophilic PU copolymers containing PEG that had ultralow Fg adsorption also had very low platelet adhesion, some of the more hydrophobic PUs had relatively high Fg adsorption but still exhibited lower platelet adhesion. To examine why some PUs with high Fg adsorption had lower platelet adhesion, three monoclonal antibodies (mAbs) that bind to sites in Fg thought to mediate platelet adhesion were used. The antibodies were: M1, specific to gamma-chain C-terminal; and R1 and R2, specific to RGD containing regions in the alpha-chain N- and C-terminal, respectively. Platelet adhesion was well correlated with M1 binding, but not with R1 or R2 binding. When these mAbs were incubated with plasma preadsorbed surfaces, they blocked adhesion to variable degrees. The ability of the R1 and R2 mAbs to partially block adhesion to adsorbed Fg suggests that RGD sites in the alpha chain may also be involved in mediating platelet adhesion and act synergistically with the C-terminal of the gamma-chain.

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Source
http://dx.doi.org/10.1002/jbm.a.30381DOI Listing

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