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An autosomal recessive gene that delays expression of lupus in BXSB mice.

R Kofler, P J McConahey, M A Duchosal, R S Balderas, A N Theofilopoulos and F J Dixon
J Immunol February 15, 1991, 146 (4) 1375-1379;
R Kofler
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P J McConahey
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M A Duchosal
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R S Balderas
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A N Theofilopoulos
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F J Dixon
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Abstract

We report the generation and serologic, cellular, histologic, and genetic characteristics of a BXSB/MpJScr substrain, termed BXSB/MpJScr-ll/ll, that has lost early-life male lupus disease. Classic genetic analysis suggested that delayed disease expression results from the action of a single autosomal recessive gene. This putative gene, referred to as ll (long-lived), causes a significant delay in expression of autoimmune serology (total serum IgG and anti-nuclear antibodies levels), monocytosis, and of immune complex-mediated histopathologic changes such as glomerulonephritis, arteritis, and myocardial infarction. Presumably as a consequence of the delayed immunopathology male BXSB/MpJScr-ll/ll mice live three to four times longer than regular BXSB/MpJScr. This strain might be useful for analysis of single genes responsible for severe autoimmune disease expression.

  • Copyright © 1991 by American Association of Immunologists

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The Journal of Immunology
Vol. 146, Issue 4
15 Feb 1991
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An autosomal recessive gene that delays expression of lupus in BXSB mice.
R Kofler, P J McConahey, M A Duchosal, R S Balderas, A N Theofilopoulos, F J Dixon
The Journal of Immunology February 15, 1991, 146 (4) 1375-1379;

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An autosomal recessive gene that delays expression of lupus in BXSB mice.
R Kofler, P J McConahey, M A Duchosal, R S Balderas, A N Theofilopoulos, F J Dixon
The Journal of Immunology February 15, 1991, 146 (4) 1375-1379;
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Print ISSN 0022-1767        Online ISSN 1550-6606