Naive and memory human B cells have distinct requirements for STAT3 activation to differentiate into antibody-secreting plasma cells

نویسندگان

  • Elissa K. Deenick
  • Danielle T. Avery
  • Anna Chan
  • Lucinda J. Berglund
  • Megan L. Ives
  • Leen Moens
  • Jennifer L. Stoddard
  • Jacinta Bustamante
  • Stephanie Boisson-Dupuis
  • Miyuki Tsumura
  • Masao Kobayashi
  • Peter D. Arkwright
  • Diana Averbuch
  • Dan Engelhard
  • Joachim Roesler
  • Jane Peake
  • Melanie Wong
  • Stephen Adelstein
  • Sharon Choo
  • Joanne M. Smart
  • Martyn A. French
  • David A. Fulcher
  • Matthew C. Cook
  • Capucine Picard
  • Anne Durandy
  • Christoph Klein
  • Steven M. Holland
  • Gulbu Uzel
  • Jean-Laurent Casanova
  • Cindy S. Ma
  • Stuart G. Tangye
چکیده

Long-lived antibody memory is mediated by the combined effects of long-lived plasma cells (PCs) and memory B cells generated in response to T cell-dependent antigens (Ags). IL-10 and IL-21 can activate multiple signaling pathways, including STAT1, STAT3, and STAT5; ERK; PI3K/Akt, and potently promote human B cell differentiation. We previously showed that loss-of-function mutations in STAT3, but not STAT1, abrogate IL-10- and IL-21-mediated differentiation of human naive B cells into plasmablasts. We report here that, in contrast to naive B cells, STAT3-deficient memory B cells responded to these STAT3-activating cytokines, differentiating into plasmablasts and secreting high levels of IgM, IgG, and IgA, as well as Ag-specific IgG. This was associated with the induction of the molecular machinery necessary for PC formation. Mutations in IL21R, however, abolished IL-21-induced responses of both naive and memory human B cells and compromised memory B cell formation in vivo. These findings reveal a key role for IL-21R/STAT3 signaling in regulating human B cell function. Furthermore, our results indicate that the threshold of STAT3 activation required for differentiation is lower in memory compared with naive B cells, thereby identifying an intrinsic difference in the mechanism underlying differentiation of naive versus memory B cells.

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عنوان ژورنال:

دوره 210  شماره 

صفحات  -

تاریخ انتشار 2013