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Comparison of antigen-specific T cell responses in autoimmune MRL/Mp-lpr/lpr and MRL/Mp-+/+ mice.

C F Scott Jr, M Tsurufuji, C Y Lu, R Finberg and M S Sy
J Immunol February 1, 1984, 132 (2) 633-639;
C F Scott Jr
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M Tsurufuji
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C Y Lu
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R Finberg
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M S Sy
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Abstract

The MRL-1 mouse develops severe autoimmune disease characterized by high titers of autoantibodies at an early age (3 to 5 mo). The congeneic MRL-n mouse, which differs only in the lymphoproliferative (lpr) gene, exhibits no such pathologic or serologic abnormalities at the same age. We examined antigen-specific T cell responses in the MRL-1 mouse and compared them to age- and sex-matched MRL-n controls. We found broad defects in these responses in the MRL-1 mouse; an inability to generate primary allospecific and hapten-specific cytolytic T lymphocytes (CTL), secondary hapten- and virus-specific CTL, as well as a deficient proliferative response to hapten and natural antigens and a weak delayed-type hypersensitivity response were demonstrated. Our data furthermore suggest a lack of interleukin 2 (IL 2) acceptor sites in the proliferating T cell, while suggesting no such lack on CTL precursors. In fact, the deficient CTL responses in MRL-1 mice can be restored to levels seen in MRL-n by the in vitro addition of IL 2. The implications of these findings and the possible explanations for the relative deficit in helper function in the MRL-1 mouse are discussed.

  • Copyright © 1984 by American Association of Immunologists

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The Journal of Immunology
Vol. 132, Issue 2
1 Feb 1984
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Comparison of antigen-specific T cell responses in autoimmune MRL/Mp-lpr/lpr and MRL/Mp-+/+ mice.
C F Scott, M Tsurufuji, C Y Lu, R Finberg, M S Sy
The Journal of Immunology February 1, 1984, 132 (2) 633-639;

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Comparison of antigen-specific T cell responses in autoimmune MRL/Mp-lpr/lpr and MRL/Mp-+/+ mice.
C F Scott, M Tsurufuji, C Y Lu, R Finberg, M S Sy
The Journal of Immunology February 1, 1984, 132 (2) 633-639;
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Print ISSN 0022-1767        Online ISSN 1550-6606