Haematologica (Jan 2008)

Factor VIII bypasses CD91/LRP for endocytosis by dendritic cells leading to T-cell activation

  • Suryasarathi Dasgupta,
  • Ana Maria Navarrete,
  • Sebastien André,
  • Bharath Wootla,
  • Sandrine Delignat,
  • Yohann Repessé,
  • Jagadeesh Bayry,
  • Antonino Nicoletti,
  • Evgueni L. Saenko,
  • Roseline d’Oiron,
  • Marc Jacquemin,
  • Jean-Marie Saint-Remy,
  • Srini V. Kaveri,
  • Sebastien Lacroix-Desmazes

DOI
https://doi.org/10.3324/haematol.11535
Journal volume & issue
Vol. 93, no. 1

Abstract

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Background The development of factor VIII (FVIII) inhibitors remains the major hurdle in the clinical management of patients with hemophilia A. FVIII uptake by professional antigen-presenting cells (APC) is the first step involved in initiation of immune responses to FVIII. Studies on FVIII catabolism have highlighted the role played by CD91/LRP as a potential target for increasing FVIII half-life in patients and prolonging treatment efficiency. We investigated the involvement of CD91 in FVIII endocytosis by human dendritic cells (DC), a model of professional APC.Design and Methods Immature DC were generated from circulating monocytes from healthy donors. Surface expression of CD91 was assessed by flow cytometry. Uptake of fluoroscein isothiocyanate-conjugated ligands by immature DC was studied in the presence of various blocking agents.Results CD91 was expressed on approximately 20% of DC and mediated the internalization of its model ligand, α2-macroglobulin. DC internalized FVIII and activated a human FVIII-specific T-cell clone in a dose-dependent manner. FVIII uptake by DC and subsequent T-cell activation were not inhibited by receptor-associated protein.Conclusions Our results indicate that CD91 and other members of the LDL receptor family are not strongly implicated in FVIII internalization by monocyte-derived DC, and suggest the involvement of alternative divalent ion-dependent endocytic receptors.