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Pathogenic role for skin macrophages in a mouse model of keratinocyte-induced psoriasis-like skin inflammation
Athanasios Stratis, … , Thomas Krieg, Ingo Haase
Athanasios Stratis, … , Thomas Krieg, Ingo Haase
Published August 1, 2006
Citation Information: J Clin Invest. 2006;116(8):2094-2104. https://doi.org/10.1172/JCI27179.
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Research Article Dermatology

Pathogenic role for skin macrophages in a mouse model of keratinocyte-induced psoriasis-like skin inflammation

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Abstract

Psoriasis is a common skin disease, the pathogenesis of which has not yet been resolved. In mice, epidermis-specific deletion of inhibitor of NF-κB (IκB) kinase 2 (IKK2) results in a skin phenotype that mimics human psoriasis in several aspects. Like psoriasis, this skin disease shows pronounced improvement when mice are treated with a TNF-neutralizing agent. We have found previously that this phenotype does not depend on the presence of αβ T lymphocytes. In order to evaluate contributions of other immune cell populations to the skin disease, we selectively eliminated macrophages and granulocytes from the skin of mice with epidermis-specific deletion of IKK2 (K14-Cre-IKK2fl/fl mice). Elimination of skin macrophages by subcutaneous injection of clodronate liposomes was accompanied by inhibition of granulocyte migration into the skin and resulted in a dramatic attenuation of psoriasis-like skin changes. The hyperproliferative, inflammatory skin disease in K14-Cre-IKK2fl/fl mice was a direct consequence of the presence of macrophages in the skin, as targeted deletion of CD18, which prevented accumulation of granulocytes but not macrophages, did not lead to major changes in the phenotype. Targeted deletion of the receptor for IFN-γ revealed that the pathogenesis of the skin disease does not depend on classical IFN-γ–mediated macrophage activation. Our results demonstrate that in mice epidermal keratinocytes can initiate a hyperproliferative, inflammatory, IFN-γ–independent, psoriasis-like skin disease whose development requires essential contributions from skin macrophages but not from granulocytes or αβ T lymphocytes.

Authors

Athanasios Stratis, Manolis Pasparakis, Rudolf A. Rupec, Doreen Markur, Karin Hartmann, Karin Scharffetter-Kochanek, Thorsten Peters, Nico van Rooijen, Thomas Krieg, Ingo Haase

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Figure 6

Elimination of granulocytes from the skin of K14-Cre-IKK2fl/fl mice does not prevent the development of the psoriasis-like skin disease.

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                  Elimination of granulocytes from the skin of K14-Cre-...
Light microscopical (top 4 panels) and confocal images (bottom 12 panels) of paraffin-embedded skin sections obtained from mice of the indicated genotypes at P7. For immunostainings, indicated markers are stained green, and nuclei are stained red. Scale bars: 100 μm (H&E); 40 μm (immunostaining).

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