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Hirochika Toyama, Seiji Okada, Masahiko Hatano, Yoshimasa Takahashi, Nobue Takeda, Hirohito Ichii, Toshitada Takemori, Yoshikazu Kuroda and Takeshi Tokuhisa
SummaryAfter immunization with T cell-dependent antigens, the high-affinity B cells selected in germinal centers differentiate into memory B cells or long-lived antibody-forming cells. However, a role for germinal centers in development of these B lineage cells is still controversial. We show here that Bcl6-deficient B cells, which cannot develop germinal centers, differentiated into IgM and IgG1 memory B cells in the spleen but barely differentiated into long-lived IgG1 antibody-forming cells in the bone marrow. Mutation in the gene was null in these memory B cells. Therefore, Bcl6 and germinal center formation are essential for somatic hypermutation, and generation of memory B cells can occur independently of germinal center formation, somatic hypermutation, and Ig class switching.
Summary | Full Text | PDF (250 kb) - Toll-like Receptor 7 and TLR9 Dictate Autoantibody Specifici...Toll-like Receptor 7 and TLR9 Dictate Autoantibody Specificity and Have Opposing Inflammatory and Regulatory Roles in a Murine Model of Lupus
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Sean R. Christensen, Jonathan Shupe, Kevin Nickerson, Michael Kashgarian, Richard A. Flavell and Mark J. Shlomchik
SummaryAntibodies (Abs) to RNA- and DNA-containing autoantigens are characteristic of systemic lupus erythematosus (SLE). We showed previously that Toll-like receptor (TLR) 9, recognizing DNA, is required for the spontaneous generation of DNA autoantibodies, but not for the development of lupus nephritis in susceptible mice. We report that lupus-prone mice deficient in TLR7, a receptor for ssRNA, failed to generate Abs to RNA-containing antigens (Ags) such as Smith (Sm) Ag. TLR9 and TLR7 also had dramatic effects on clinical disease in lupus-prone mice. In the absence of TLR9, autoimmune disease was exacerbated, lymphocytes and plasmacytoid DCs were more activated, and serum IgG and IFN-α were increased. In contrast, TLR7-deficient mice had ameliorated disease, decreased lymphocyte activation, and decreased serum IgG. These findings reveal opposing inflammatory and regulatory roles for TLR7 and TLR9, despite similar tissue expression and signaling pathways. These results have important implications for TLR-directed therapy of autoimmune disease.
Summary | Full Text | PDF (763 kb) - Cbl-b Is a Negative Regulator of Receptor Clustering and Raf...Cbl-b Is a Negative Regulator of Receptor Clustering and Raft Aggregation in T Cells
Immunity, Volume 13, Issue 4, 1 October 2000, Pages 463-473
Connie Krawczyk, Kurt Bachmaier, Takehiko Sasaki, Russell G Jones, Scott B Snapper, Dennis Bouchard, Ivona Kozieradzki, Pamela S Ohashi, Frederick W Alt and Josef M Penninger
SummaryStimulation of T cells via the antigen and costimulatory receptors leads to the organization of a supramolecular activation cluster called the immune synapse. We report that loss of the molecular adaptor Cbl-b in T cells frees antigen receptor–triggered receptor clustering, lipid raft aggregation, and sustained tyrosine phosphorylation from the requirement for CD28 costimulation. Introduction of the mutation into a background relieved the functional defects of T cells and caused spontaneous autoimmunity. Wiscott Aldrich Syndrome protein (WASP) was found to be essential for deregulated proliferation and membrane receptor reorganization of mutant T cells. Antigen receptor–triggered Ca mobilization, cytokine production, and receptor clustering can be genetically uncoupled in mutant T cells. Thus, Cbl-b functions as a negative regulator of receptor clustering and raft aggregation in T cells.
Summary | Full Text | PDF (1068 kb) - …more
Copyright © 1995 The Biophysical Society. All rights reserved.
Biophysical Journal, Volume 68, Issue 3, 1170-1176, 1 March 1995
doi:10.1016/S0006-3495(95)80293-6
Research Article
Cross-linking of CD4 in a TCR/CD3-juxtaposed inhibitory state: a pFRET study
G. Szabó, J.L. Weaver, P.S. Pine, P.E. Rao and A. Aszalos
Department of Biophysics, University Medical School of Debrecen, Hungary.
Abstract
Instances when T cell activation via the T cell receptor/CD3 complex is suppressed by anti-CD4 Abs are generally attributed either to the topological separation of CD4-p56lck from CD3, or their improper apposition. Photobleaching fluorescence resonance energy transfer measurements permitted direct analysis of these alternatives on human peripheral blood lymphocytes. Distinction between changes of relative antigen densities or positioning was made possible by simultaneously recording donor and acceptor fluorescence in the energy transfer experiment performed on homogeneous populations of flow-sorted cells. We show here that CD4 stays in the molecular vicinity of CD3, while anti-CD3 stimulation is suppressed by anti-CD4 or cross-linked HIV gp120. Our data suggest that cross-linking of CD4 through particular epitopes is capable of inhibiting activation driven by Abs binding to specific sites on CD3 without major topological sequestration of the Ags, in such a way that additional positive signals will also be affected. Thus, these and other related cases of negative signaling via CD4 may be interpreted in terms of functional uncoupling rather than a wide physical separation of CD4 from the T cell receptor-CD3 complex.
