Abstract

The dramatic clinical response of psoriasis to cyclosporin A has rekindled interest in the role of the immune system in psoriasis, a skin disease which affects 1-2% of the American population. The principal objective of this proposal is to take a fresh look at the role of the immune system in the etiopathogenesis of psoriasis at the molecular biochemical level by studying specific interactions between peripheral blood mononuclear leukocytes (PBML) and keratinocytes (KCs) both in vitro and in vivo with particular emphasis on gamma interferon (IFN-gamma). Focus on IFN- gamma is justified because it influences KC growth and differentiation, both of which are altered in psoriasis and because of our ability to measure functional, high affinity receptors for IFN-gamma on normal KCs by ligand binding studies which will facilitate detection of any KC IFN-gamma membrane receptor abnormalities in psoriasis. Since IFN gamma inhibits the proliferation of normal KCs and induces HLA-DR expression to 10-11M, our hypothesis is: In psoriasis, the epidermal hyperplasia and lack of KC HLA-DR expression is a reflection of either inadequate tissue levels of IFN-gamma or an altered KC response to IFN-gamma because of abnormal KC IFN-gamma membrane receptors, which leads to perpetuation of the immunobiological alterations characteristic of psoriasis. Direct PBML/KC cellular interactions which may be important in the early initiating phases of psoriasis will be studied using a simple in vitro adherence assay to investigate the molecular mechanisms of recognition and binding involved between PBML and KC. We propose to integrate immunological, biochemical and cell surface (receptor and adherence molecule) perspectives in psoriasis by dissecting specific PBML/KC interactions and by focusing on early cellular reactions which may occur in the initiation of a psoriatic lesion and the soluble mediators produced following the onset of the inflammatory process. Our simplified working model for psoriasis is similar to that proposed by Fry et al (Imm Tod 7:256, 1986): 1) Psoriasis is triggered by the appearance of a putative psoriasis antigen (related to streptococcal or viral antigen, drugs, trauma, etc.) with initiation of tissue injury. 2) There is early macrophage-T cell interaction to """"""""antigen"""""""" with PBML activation and production of lymphokines (IL-1, IL-2, etc. - which may be inhibited by cyclosporin A). 3) There is infiltration into epidermis with adherence of PBML to KCs with perpetuation of """"""""microwounding"""""""" and further release of lymphokines, some of which may stimulate KC repair (i.e., IL-1) and others which inhibit KC proliferation (i.e. IFN-gamma). 4) The reparative KC hyperplasia """"""""overshoots"""""""" and hyperproliferation dominates because of either a) low IFN- gamma levels or b) altered KC IFN-gamma receptors (either intrinsic or acquired from neutrophil/mast cell proteinases, for example). This scenario would be consistent with the Koebner reaction, the clinical responsiveness to cyclosporin A and the immunohistological features of psoriasis. Our results should not only yield valuable information with respect to psoriasis, but also aid in our understanding and treatment of many other inflammatory skin diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
First Independent Research Support & Transition (FIRST) Awards (R29)
Project #
5R29AR038957-02
Application #
3456934
Study Section
General Medicine A Subcommittee 2 (GMA)
Project Start
1987-09-01
Project End
1990-08-31
Budget Start
1988-09-01
Budget End
1989-08-31
Support Year
2
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Gutierrez-Steil, C; Wrone-Smith, T; Sun, X et al. (1998) Sunlight-induced basal cell carcinoma tumor cells and ultraviolet-B-irradiated psoriatic plaques express Fas ligand (CD95L). J Clin Invest 101:33-9
Mitra, R S; Wrone-Smith, T; Simonian, P et al. (1997) Apoptosis in keratinocytes is not dependent on induction of differentiation. Lab Invest 76:99-107
Wrone-Smith, T; Mitra, R S; Thompson, C B et al. (1997) Keratinocytes derived from psoriatic plaques are resistant to apoptosis compared with normal skin. Am J Pathol 151:1321-9
Wrone-Smith, T; Nickoloff, B J (1996) Dermal injection of immunocytes induces psoriasis. J Clin Invest 98:1878-87
Wrone-Smith, T; Johnson, T; Nelson, B et al. (1995) Discordant expression of Bcl-x and Bcl-2 by keratinocytes in vitro and psoriatic keratinocytes in vivo. Am J Pathol 146:1079-88
Nestle, F O; Nickoloff, B J (1994) Role of dendritic cells in benign and malignant lymphocytic infiltrates of the skin. Dermatol Clin 12:271-82
Nickoloff, B J; Mitra, R S; Varani, J et al. (1994) Aberrant production of interleukin-8 and thrombospondin-1 by psoriatic keratinocytes mediates angiogenesis. Am J Pathol 144:820-8
Goodman, R E; Nestle, F; Naidu, Y M et al. (1994) Keratinocyte-derived T cell costimulation induces preferential production of IL-2 and IL-4 but not IFN-gamma. J Immunol 152:5189-98
Nestle, F O; Thompson, C; Shimizu, Y et al. (1994) Costimulation of superantigen-activated T lymphocytes by autologous dendritic cells is dependent on B7. Cell Immunol 156:220-9
Nickoloff, B J; Mitra, R S; Lee, K et al. (1993) Discordant expression of CD28 ligands, BB-1, and B7 on keratinocytes in vitro and psoriatic cells in vivo. Am J Pathol 142:1029-40

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