Males from the BXSB murine strain (H-2b) spontaneously develop an autoimmune syndrome with features of systemic lupus erythematosus (SLE), which results in part from the action of a mutant gene (Yaa) located on the Y chromosome. Like other H-2b mice, the BXSB strain does not express the class II major histocompatibility complex antigen, I-E. Here we report that the expression of I-E (E alpha dE beta b) in BXSB males bearing an E alpha d transgene prevents hypergammaglobulinemia, autoantibody production, and subsequent autoimmune glomerulonephritis. These transgenic mice bear on the majority of their B cells not only I-E molecules, but also an I-E alpha chain-derived peptide presented by a higher number of I-Ab molecules, as recognized by the Y-Ae monoclonal antibody. The I-E+ B cells appear less activated in vivo than the I-E- B cells, a minor population. This limited activation of the I-E+ B cells does not reflect a functional deficiency of this cell population, since it can be stimulated to IgM production in vitro by lipopolysaccharides at an even higher level than the I-E- B cell population. The development of the autoimmune syndrome in the transgenic and nontransgenic bone marrow chimeric mice argues against the possibility that the induction of regulatory T cells or clonal deletion of potential autoreactive T cells as a result of I-E expression is a mechanism of the protection conferred by the E alpha d transgene. We propose a novel mechanism by which the E alpha d transgene protects BXSB mice against SLE: overexpression of I-E alpha chains results in the generation of excessive amounts of a peptide displaying a high affinity to the I-Ab molecule, thereby competing with pathogenic autoantigen-derived peptides for presentation by B lymphocytes and preventing their excessive stimulation.
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1 October 1993
Article|
October 01 1993
Prevention of systemic lupus erythematosus in autoimmune BXSB mice by a transgene encoding I-E alpha chain.
R Merino,
R Merino
Department of Pathology, University of Geneva, Switzerland.
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M Iwamoto,
M Iwamoto
Department of Pathology, University of Geneva, Switzerland.
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L Fossati,
L Fossati
Department of Pathology, University of Geneva, Switzerland.
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P Muniesa,
P Muniesa
Department of Pathology, University of Geneva, Switzerland.
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K Araki,
K Araki
Department of Pathology, University of Geneva, Switzerland.
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S Takahashi,
S Takahashi
Department of Pathology, University of Geneva, Switzerland.
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J Huarte,
J Huarte
Department of Pathology, University of Geneva, Switzerland.
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K Yamamura,
K Yamamura
Department of Pathology, University of Geneva, Switzerland.
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J D Vassalli,
J D Vassalli
Department of Pathology, University of Geneva, Switzerland.
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S Izui
S Izui
Department of Pathology, University of Geneva, Switzerland.
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R Merino
Department of Pathology, University of Geneva, Switzerland.
M Iwamoto
Department of Pathology, University of Geneva, Switzerland.
L Fossati
Department of Pathology, University of Geneva, Switzerland.
P Muniesa
Department of Pathology, University of Geneva, Switzerland.
K Araki
Department of Pathology, University of Geneva, Switzerland.
S Takahashi
Department of Pathology, University of Geneva, Switzerland.
J Huarte
Department of Pathology, University of Geneva, Switzerland.
K Yamamura
Department of Pathology, University of Geneva, Switzerland.
J D Vassalli
Department of Pathology, University of Geneva, Switzerland.
S Izui
Department of Pathology, University of Geneva, Switzerland.
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1993) 178 (4): 1189–1197.
Citation
R Merino, M Iwamoto, L Fossati, P Muniesa, K Araki, S Takahashi, J Huarte, K Yamamura, J D Vassalli, S Izui; Prevention of systemic lupus erythematosus in autoimmune BXSB mice by a transgene encoding I-E alpha chain.. J Exp Med 1 October 1993; 178 (4): 1189–1197. doi: https://doi.org/10.1084/jem.178.4.1189
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