Suppressive functions of activated B cells in autoimmune diseases reveal the dual roles of Toll-like receptors in immunity

  1. Vicky Lampropoulou1,
  2. Elisabeth Calderon-Gomez1,
  3. Toralf Roch1,
  4. Patricia Neves1,
  5. Ping Shen1,
  6. Ulrik Stervbo1,
  7. Pierre Boudinot2,
  8. Stephen M. Anderton3,
  9. Simon Fillatreau1

Article first published online: 23 DEC 2009

DOI: 10.1111/j.0105-2896.2009.00855.x

Issue

Immunological Reviews

Immunological Reviews

Special Issue: Inflammatory Arthritis

Volume 233, Issue 1, pages 146–161, January 2010

Additional Information

How to Cite

Lampropoulou, V., Calderon-Gomez, E., Roch, T., Neves, P., Shen, P., Stervbo, U., Boudinot, P., Anderton, S. M. and Fillatreau, S. (2010), Suppressive functions of activated B cells in autoimmune diseases reveal the dual roles of Toll-like receptors in immunity. Immunological Reviews, 233: 146–161. doi: 10.1111/j.0105-2896.2009.00855.x

Author Information

  1. 1

    Laboratory of immune regulation, Deutsches Rheuma-Forschungszentrum, Berlin, Germany.

  2. 2

    Virologie et Immunologie Moléculaires, INRA, Jouy-en-Josas, France.

  3. 3

    Centre for Inflammation Research and Centre for Multiple Sclerosis Research, Queen’s Medical research Institute, University of Edinburgh, Edinburgh, United Kingdom.

*S. Fillatreau Deutsches Rheuma-Forschungszentrum Chariteplatz 1 10117 Berlin Germany Tel.: +49 0 30 284 60 752 Fax: +49 0 30 284 60 603 e-mail: fillatreau@drfz.de

Publication History

  1. Issue published online: 23 DEC 2009
  2. Article first published online: 23 DEC 2009

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Keywords:

  • B cells;
  • autoimmunity;
  • Toll-like receptor;
  • interleukin-10;
  • immunoregulation;
  • feedforward loop

Summary:  B lymphocytes contribute to immunity through production of antibodies, antigen presentation to T cells, and secretion of cytokines. B cells are generally considered in autoimmune diseases as drivers of pathogenesis. This view is certainly justified, given the successful utilization of the B cell-depleting reagent rituximab in patients with rheumatoid arthritis or other autoimmune pathologies. In a number of cases, however, the depletion of B cells led to an exacerbation of symptoms in patients with autoimmune disorders. In a similar manner, mice lacking B cells can develop an aggravated course of disease in several autoimmune models. These paradoxical observations are now explained by the concept that activated B cells can suppress immune responses through the production of cytokines, especially interleukin-10. Here, we review the stimulatory signals that induce interleukin-10 secretion and suppressive functions in B cells and the phenotype of the B cells with such characteristics. Finally, we formulate a model explaining how this process of immune regulation by activated B cells can confer advantageous properties to the immune system in its combat with pathogens. Altogether, this review proposes that B-cell-mediated regulation is a fundamental property of the immune system, with features of great interest for the development of new cell-based therapies for autoimmune diseases.

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