The expression of Fc epsilon R on human lymphocytes was studied with the anti-Fc epsilon R mAbs. Fc epsilon R was expressed on most mu+,delta+ circulating B cells, whereas T cells did not express Fc epsilon R even in patients with hyper-IgE syndrome. B cells with gamma, alpha, or epsilon phenotype did not express Fc epsilon R, moreover its expression could not be induced, suggesting that the Fc epsilon R expression was correlated with isotype switching. mu+delta+ B cells in bone marrow did not express Fc epsilon R, but PHA-sup (supernatant from PHA-stimulated cell cultures) could induce its expression, and the addition of IgE augmented this induction. Recombinant IL-2, IL-1, IFN-gamma or -beta, or purified B cell differentiation factor (BSF-2 B cell-stimulatory factor 2) could not induce Fc epsilon R expression in bone marrow B cells. IFN-gamma inhibited the Fc epsilon R expression induced by PHA-sup, suggesting that the human counterpart of BSF-1 may be responsible for Fc epsilon R expression in bone marrow B cells. B cells from patients with common variable immunodeficiency and ataxia telangiectasia did not express Fc epsilon R, but PHA-sup could induce its expression, indicating that circulating B cells of these patients are at a differentiation stage similar to B cells in bone marrow. The study showed that Fc epsilon R is a B cell-specific differentiation marker, the expression of which is restricted to a defined stage of B cell differentiation.
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1 November 1986
Article|
November 01 1986
Fc epsilon receptor, a specific differentiation marker transiently expressed on mature B cells before isotype switching.
H Kikutani
M Suemura
H Owaki
H Nakamura
R Sato
K Yamasaki
E L Barsumian
R R Hardy
T Kishimoto
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1986) 164 (5): 1455–1469.
Citation
H Kikutani, M Suemura, H Owaki, H Nakamura, R Sato, K Yamasaki, E L Barsumian, R R Hardy, T Kishimoto; Fc epsilon receptor, a specific differentiation marker transiently expressed on mature B cells before isotype switching.. J Exp Med 1 November 1986; 164 (5): 1455–1469. doi: https://doi.org/10.1084/jem.164.5.1455
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