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Cross-Linking GPVI-Fc by Anti-Fc Antibodies Potentiates Its Inhibition of Atherosclerotic Plaque- and Collagen-Induced Platelet Activation

  • Janina Jamasbi
  • , Remco T.A. Megens
  • , Mariaelvy Bianchini
  • , Kerstin Uhland
  • , Götz Münch
  • , Martin Ungerer
  • , Shachar Sherman
  • , Alexander Faussner
  • , Richard Brandl
  • , Christine John
  • , Johannes Buchner
  • , Christian Weber
  • , Reinhard Lorenz
  • , Natalie Elia
  • , Wolfgang Siess
  • University of Munich
  • Maastricht University
  • advanceCOR GmbH
  • Ben Gurion University of the Negev
  • St. Mary's Square Institute for Vascular Surgery and Phlebology
  • Technical University of Munich
  • Partner Site Munich Heart Alliance

Research output: Contribution to journalReview articlepeer-review

17 Scopus citations

Abstract

To enhance the antithrombotic properties of recombinant glycoprotein VI fragment crystallizable (GPVI-Fc), the authors incubated GPVI-Fc with anti-human Fc antibodies to cross-link the Fc tails of GPVI-Fc. Cross-linking potentiated the inhibition of human plaque- and collagen-induced platelet aggregation by GPVI-Fc under static and flow conditions without increasing bleeding time in vitro. Cross-linking with anti-human-Fc Fab2 was even superior to anti-human-Fc immunoglobulin G (IgG). Advanced optical imaging revealed a continuous sheath-like coverage of collagen fibers by cross-linked GPVI-Fc complexes. Cross-linking of GPVI into oligomeric complexes provides a new, highly effective, and probably safe antithrombotic treatment as it suppresses platelet GPVI-plaque interaction selectively at the site of acute atherothrombosis.

Original languageEnglish
Pages (from-to)131-142
Number of pages12
JournalJACC: Basic to Translational Science
Volume1
Issue number3
DOIs
StatePublished - 1 Apr 2016

Keywords

  • antithrombotic
  • atherothrombosis
  • glycoprotein VI
  • plaque rupture

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