TLR4- and TRIF-dependent stimulation of B lymphocytes by peptide liposomes enables T cell-independent isotype switch in mice.

نویسندگان

  • Maria Pihlgren
  • Alberto B Silva
  • Rime Madani
  • Valérie Giriens
  • Ying Waeckerle-Men
  • Antonia Fettelschoss
  • David T Hickman
  • María Pilar López-Deber
  • Dorin Mlaki Ndao
  • Marija Vukicevic
  • Anna Lucia Buccarello
  • Valérie Gafner
  • Nathalie Chuard
  • Pedro Reis
  • Kasia Piorkowska
  • Andrea Pfeifer
  • Thomas M Kündig
  • Andreas Muhs
  • Pål Johansen
چکیده

Immunoglobulin class switching from IgM to IgG in response to peptides is generally T cell-dependent and vaccination in T cell-deficient individuals is inefficient. We show that a vaccine consisting of a dense array of peptides on liposomes induced peptide-specific IgG responses totally independent of T-cell help. Independency was confirmed in mice lacking T cells and in mice deficient for MHC class II, CD40L, and CD28. The IgG titers were high, long-lived, and comparable with titers obtained in wild-type animals, and the antibody response was associated with germinal center formation, expression of activation-induced cytidine deaminase, and affinity maturation. The T cell-independent (TI) IgG response was strictly dependent on ligation of TLR4 receptors on B cells, and concomitant TLR4 and cognate B-cell receptor stimulation was required on a single-cell level. Surprisingly, the IgG class switch was mediated by TIR-domain-containing adapter inducing interferon-β (TRIF), but not by MyD88. This study demonstrates that peptides can induce TI isotype switching when antigen and TLR ligand are assembled and appropriately presented directly to B lymphocytes. A TI vaccine could enable efficient prophylactic and therapeutic vaccination of patients with T-cell deficiencies and find application in diseases where induction of T-cell responses contraindicates vaccination, for example, in Alzheimer disease.

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Regular Article IMMUNOBIOLOGY TLR4- and TRIF-dependent stimulation of B lymphocytes by peptide liposomes enables T cell–independent isotype switch in mice

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عنوان ژورنال:
  • Blood

دوره 121 1  شماره 

صفحات  -

تاریخ انتشار 2013