Fabio Ghiotto, Franco Fais, Angelo Valetto, Emilia Albesiano, Shiori Hashimoto, Mariella Dono, Hideyuki Ikematsu, Steven L. Allen, Jonathan Kolitz, Kanti R. Rai, Marco Nardini, Anna Tramontano, Manlio Ferrarini, Nicholas Chiorazzi
J Clin Invest.
2004;
113(7):1008–1016
doi:10.1172/JCI19399
This article Copyright © 2004, The American Society for Clinical Investigation
Abstract
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S
tudies of B cell antigen receptors (BCRs) expressed by leukemic lymphocytes from
patients with B cell chronic lymphocytic leukemia (B-CLL) suggest that B
lymphocytes with some level of BCR structural restriction become transformed.
While analyzing rearranged VHDJH and
VLJL genes of 25 non–IgM-producing B-CLL
cases, we found five IgG+ cases that display strikingly
similar BCRs (use of the same H- and L-chain V gene segments with unique, shared
heavy chain third complementarity-determining region
[HCDR3] and light chain third
complementarity-determining region [LCDR3] motifs).
These H- and L-chain characteristics were not identified in other B-CLL cases or
in normal B lymphocytes whose sequences are available in the public databases.
Three-dimensional modeling studies suggest that these BCRs could bind the same
antigenic epitope. The structural features of the B-CLL BCRs resemble those of
mAb’s reactive with carbohydrate determinants of bacterial capsules
or viral coats and with certain autoantigens. These findings suggest that the B
lymphocytes that gave rise to these IgG+ B-CLL cells were
selected for this unique BCR structure. This selection could have occurred
because the precursors of the B-CLL cells were chosen for their antigen-binding
capabilities by antigen(s) of restricted nature and structure, or because the
precursors derived from a B cell subpopulation with limited BCR heterogeneity,
or both.
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