4.6 Article

Microparticles (Ectosomes) Shed by Stored Human Platelets Downregulate Macrophages and Modify the Development of Dendritic Cells

Journal

JOURNAL OF IMMUNOLOGY
Volume 186, Issue 11, Pages 6543-6552

Publisher

AMER ASSOC IMMUNOLOGISTS
DOI: 10.4049/jimmunol.1002788

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Funding

  1. Swiss National Foundation [32000-116839]
  2. Roche Foundation for Anemia Research
  3. Fondazione per la ricerca sulla trasfusione e sui trapianti (Lugano, Switzerland)
  4. Nora van Meeuwen Stiftung

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Microparticles (MP) shed by platelets (PLT) during storage have procoagulant activities, but little is known about their properties to modify inflammation or immunity. In this study, we studied the capacity of MP present in PLT concentrates to alter the function of macrophages and dendritic cells (DC). The size of the purified MP was between 100 and 1000 nm, and they expressed phosphatidylserine; surface proteins of PLT (CD61, CD36, CD47), including complement inhibitors (CD55, CD59), but not CD63; and proteins acquired from plasma (C1q, C3 fragments, factor H). These characteristics suggest that the MP shed by PLT are formed by budding from the cell surface, corresponding to ectosomes. The purified PLT ectosomes (PLT-Ect) reduced the release of TNF-alpha and IL-10 by macrophages activated with LPS or zymosan A. In addition, PLT-Ect induced the immediate release of TGF-beta from macrophages, a release that was not modified by LPS or zymosan A. Macrophages had a reduced TNF-alpha release even 24 h after their exposure to PLT-Ect, suggesting that PLT-Ect induced a modification of the differentiation of macrophages. Similarly, the conventional 6-d differentiation of monocytes to immature DC by IL-4 and GM-CSF was modified by the presence of PLT-Ect during the first 2 d. Immature DC expressed less HLA-DP DQ DR and CD80 and lost part of their phagocytic activity, and their LPS-induced maturation was downmodulated when exposed to PLT-Ect. These data indicate that PLT-Ect shed by stored PLT have intrinsic properties that modify macrophage and DC differentiation toward less reactive states. The Journal of Immunology, 2011, 186: 6543-6552.

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