CD40–CD40 ligand (L) interactions play a pivotal role in immune-mediated inflammatory responses via the activation of antigen-presenting cells (APCs). To investigate the effects of continuous activation of resident tissue APCs, in this case the Langerhans cells (LCs) of the skin, CD40L expression was targeted to the basal keratinocytes of the epidermis of mice using the keratin-14 promoter. Approximately 80% of the transgenic (Tg) mice spontaneously developed dermatitis on the ears, face, tail, and/or paws. Compared with littermates, Tgs had a >90% decrease in epidermal LCs yet increased numbers within the dermis suggestive of enhanced emigration of CD40-activated LCs. Tgs also displayed massive regional lymphadenopathy with increased numbers of dendritic cells and B cells. Moreover, a decrease in IgM and an increase in IgG1/IgG2a/IgG2b/IgE serum concentrations was detectable. Screening for autoantibodies revealed the presence of antinuclear antibodies and anti-dsDNA antibodies implicative of systemic autoimmunity. Accordingly, renal Ig deposits, proteinuria, and lung fibrosis were observed. Adoptive transfer of T cells from Tgs to nonTg recipients evoked the development of skin lesions similar to those found in the Tgs. Dermatitis also developed in B cell–deficient CD40L Tg mice. These findings suggest that in situ activation of LCs by CD40L in the skin not only leads to chronic inflammatory dermatitis but also to systemic mixed-connective-tissue-like autoimmune disorders, possibly by breaking immune tolerance against the skin.
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3 September 2001
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August 27 2001
Overexpression of Cd40 Ligand in Murine Epidermis Results in Chronic Skin Inflammation and Systemic Autoimmunity
Annette Mehling,
Annette Mehling
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Karin Loser,
Karin Loser
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Georg Varga,
Georg Varga
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Dieter Metze,
Dieter Metze
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Thomas A. Luger,
Thomas A. Luger
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Thomas Schwarz,
Thomas Schwarz
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Stephan Grabbe,
Stephan Grabbe
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Stefan Beissert
Stefan Beissert
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
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Annette Mehling
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Karin Loser
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Georg Varga
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Dieter Metze
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Thomas A. Luger
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Thomas Schwarz
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Stephan Grabbe
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Stefan Beissert
aLudwig Boltzmann Institute for Cell Biology, Department of Dermatology and Immunology of the Skin, University of Münster, D-49149 Münster, Germany
Abbreviations used in this paper: ANA, antinuclear antibody; DC, dendritic cell; H&E, hematoxylin and eosin; HRP, horseradish peroxidase; L, ligand; LC, Langerhans cell; Tg, transgenic.
Received:
January 17 2001
Revision Requested:
June 22 2001
Accepted:
July 17 2001
Online ISSN: 1540-9538
Print ISSN: 0022-1007
© 2001 The Rockefeller University Press
2001
The Rockefeller University Press
J Exp Med (2001) 194 (5): 615–628.
Article history
Received:
January 17 2001
Revision Requested:
June 22 2001
Accepted:
July 17 2001
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Citation
Annette Mehling, Karin Loser, Georg Varga, Dieter Metze, Thomas A. Luger, Thomas Schwarz, Stephan Grabbe, Stefan Beissert; Overexpression of Cd40 Ligand in Murine Epidermis Results in Chronic Skin Inflammation and Systemic Autoimmunity. J Exp Med 3 September 2001; 194 (5): 615–628. doi: https://doi.org/10.1084/jem.194.5.615
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