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The Journal of Immunology, Vol 136, Issue 3 823-829, Copyright © 1986 by American Association of Immunologists


ARTICLES

T cell development in B cell-deficient mice. IV. The role of B cells as antigen-presenting cells in vivo

KT Hayglass, SJ Naides, CF Scott Jr, B Benacerraf and MS Sy

B cell-deficient, rabbit anti-mouse IgM-treated mice were compared with normal or normal rabbit immunoglobulin-treated controls in their ability to develop proliferative T cell responses, delayed hypersensitivity, and primary or secondary cytotoxic T cell responses. Immunization with hapten-coupled autologous spleen cells resulted in anti-mu-treated mice generating only marginal T cell responses. This decreased responsiveness was shown to be attributable not to an intrinsic T cell defect or to changes in the ability of macrophages from anti-mu-treated mice to present soluble antigen, but rather to the greatly diminished capacity of B cell-deficient spleen cells to present antigen. The results support the concept that B cells play a significant role in antigen presentation required for T cell activation.


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