[HTML][HTML] The relationship between CD27 negative and positive B cell populations in human peripheral blood

YCB Wu, D Kipling, DK Dunn-Walters - Frontiers in immunology, 2011 - frontiersin.org
Frontiers in immunology, 2011frontiersin.org
CD27 expression has been used to distinguish between memory and naive B cells in
humans. However, low levels of mutated and isotype-switched CD27− IgD− cells are seen in
healthy adults, and these are increased in some autoimmune diseases and in the elderly.
Thus CD27 is not a universal marker of memory B cells in humans. Various hypotheses
have been put forward as to the function of the CD27− memory population. Since we have
previously found high-throughput IGHV repertoire analysis useful to distinguish “innate-like” …
CD27 expression has been used to distinguish between memory and naive B cells in humans. However, low levels of mutated and isotype-switched CD27−IgD− cells are seen in healthy adults, and these are increased in some autoimmune diseases and in the elderly. Thus CD27 is not a universal marker of memory B cells in humans. Various hypotheses have been put forward as to the function of the CD27− memory population. Since we have previously found high-throughput IGHV repertoire analysis useful to distinguish “innate-like” memory B cells (CD27+IgD+), we have employed similar analyses to elucidate the relationship between CD27− and CD27+ memory B cells. IgM+IgD− memory cells in both the CD27+ and CD27− compartments share the unique characteristics of the “innate-like” IgM+IgD+CD27+ cells. The switched CD27+ and CD27− memory cells share a similar IGHV repertoire, having more in common with each other than with “innate-like” memory cells, although it is interesting that IgG2 and IgA2 subclasses of antibody in both switched memory populations have a more “innate-like” repertoire. Clonality analysis shows evidence of a close clonal relationship between the two populations in that both CD27− and CD27+ switched memory cells can be found in the same genealogical tree. The expression of CD27 does not appear to occur in a linear developmental fashion, since we see CD27− cells as precursors of CD27+ cells and vice versa. Despite the similarities, the CDR-H3 repertoire of the CD27− cells is significantly different from both the CD27+IgD+ and CD27+IgD− populations, indicating that perhaps the lack of CD27 might be related to binding properties of the Ig CDR-H3 region.
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