PLoS ONE (Jan 2009)

TRAF6 is required for generation of the B-1a B cell compartment as well as T cell-dependent and -independent humoral immune responses.

  • Takashi Kobayashi,
  • Tae Soo Kim,
  • Anand Jacob,
  • Matthew C Walsh,
  • Yuho Kadono,
  • Ezequiel Fuentes-Pananá,
  • Tomoko Yoshioka,
  • Akihiko Yoshimura,
  • Masahiro Yamamoto,
  • Tsuneyasu Kaisho,
  • Shizuo Akira,
  • John G Monroe,
  • Yongwon Choi

DOI
https://doi.org/10.1371/journal.pone.0004736
Journal volume & issue
Vol. 4, no. 3
p. e4736

Abstract

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TNF receptor superfamily members, such as CD40 and the Toll-like receptors (TLRs), regulate many aspects of B cell differentiation and activation. TRAF6 is an intracellular signaling adaptor molecule for these receptors, but its role in B cells has not been clarified by previous genetic approaches, as the systemic deletion of the TRAF6 gene results in perinatal lethality. Here we show that B cell-specific TRAF6 deficiency results in a reduced number of mature B cells in the bone marrow and spleen. Optimal T cell-dependent (TD) antigen responses, as characterized by isotype switching and long-lived plasma cell generation, are also impaired in B cell-specific TRAF6-deficient mice. B cell-specific TRAF6-deficient mice also exhibit lower levels of serum IgM and IgG2b and defective antigen-specific IgM production in response to T cell-independent (TI) antigens. Unexpectedly, TRAF6-deficient B cell progenitors are unable to generate CD5(+) B-1 cells. These results reveal critical roles for TRAF6 in TD and TI humoral immune responses and in inductive fate decisions necessary to generate the B-1 B cell compartment.