Clonal deletion of autospecific B lymphocytes.
D Nemazee, D Russell, B Arnold… - Immunological …, 1991 - europepmc.org
Immunological reviews, 1991•europepmc.org
Using mice transgenic for functional, rearranged immunoglobulin heavy and light chain
genes, it can be demonstrated that B lymphocytes reactive with cell surface-bound class I
MHC antigen can be controlled by clonal elimination. Even low-affinity cell-bound ligands
can induce deletion. Deletion can occur in the pre-B to B cell transitional stage or after the B
cells exist the bone marrow, depending on where the cells first encounter autoantigen. IgD
appears to play no role in protecting cells from deletion. It is argued that defects in B-cell …
genes, it can be demonstrated that B lymphocytes reactive with cell surface-bound class I
MHC antigen can be controlled by clonal elimination. Even low-affinity cell-bound ligands
can induce deletion. Deletion can occur in the pre-B to B cell transitional stage or after the B
cells exist the bone marrow, depending on where the cells first encounter autoantigen. IgD
appears to play no role in protecting cells from deletion. It is argued that defects in B-cell …
Using mice transgenic for functional, rearranged immunoglobulin heavy and light chain genes, it can be demonstrated that B lymphocytes reactive with cell surface-bound class I MHC antigen can be controlled by clonal elimination. Even low-affinity cell-bound ligands can induce deletion. Deletion can occur in the pre-B to B cell transitional stage or after the B cells exist the bone marrow, depending on where the cells first encounter autoantigen. IgD appears to play no role in protecting cells from deletion. It is argued that defects in B-cell tolerance alone may be sufficient to lead to systemic autoimmunity.
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