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Pathomechanismen der Induktion und Aufrechterhaltung der Autoimmunantwort bei Psoriasis

Fachliche Zuordnung Dermatologie
Rheumatologie
Förderung Förderung von 2016 bis 2022
Projektkennung Deutsche Forschungsgemeinschaft (DFG) - Projektnummer 317045689
 
Erstellungsjahr 2022

Zusammenfassung der Projektergebnisse

Psoriasis is due to an immune response caused by CD8+ T cells in lesional epidermis. HLA- C*06:02 mediates the actual psoriasis-specific risk in epistasis with variants of the endoplasmic reticulum aminopeptidase 1 (ERAP1) gene. Both interact in antigen presentation. Using a pathogenic Vα3S1/Vβ13S1 T-cell receptor (TZR) from a lesional psoriatic CD8+ T-cell clone, we had uncovered that HLA-C*06:02 mediates an autoimmune response against melanocytes by presenting an autoantigenic peptide from ADAMTS-like protein 5. These results were the basis of the grant proposal. In the funded project, we now reveal that the immunogenicity of melanocytes in psoriasis and the generation of the autoantigenic ADAMTSL5 epitope from precursor peptides is ERAP1- dependent. ERAP1-knock out in melanoma cell lines completely abolished the ability to stimulate the Vα3S1/Vβ13S1 TCR. Risk haplotypes of ERAP1 enhanced melanocyte immunogenicity through increased production of the HLA-C*06:02-presented ADAMTSL5 epitope. Interestingly, HLA-C*06:02 protects from malignant melanoma. As a side aspect of the psoriatic autoimmune response against melanocytes we followed TCR diversity during checkpoint inhibition for the treatment of advanced malignant melanoma. Here we find that the extent of clonal T cell expansion prior to checkpoint inhibition is a prognostic marker for response to therapy. Psoriasis is triggered by environmental factors throughout life. Fine characterization of the peptide recognition motif of the ADAMTSL5-specific Vα3S1/Vβ13S1 T-cell receptor allowed us to identify various environmental antigens from microbiota, pathogens, tobacco, yeast and wheat as environmental triggers of psoriasis that stimulate the Vα3S1/Vβ13S1-TCR and CD8+ T cells of psoriasis patients. Through developing peptide-loaded HLA-C*06:02 tetramers, we could demonstrate that ADAMTSL5-specific CD8+ T cells are increased in the blood of psoriasis patients and may also react against wheat peptides. A wheat-free diet improved psoriasis in several patients. This opens up the possibility to establish a diseasespecific biomarker and indicates how psoriasis patients may ameliorate the disease by lifestyle changes. Generalized pustular psoriasis (GPP) is the most severe manifestation in the psoriasis spectrum. During the research period, we demonstrate that unopposed IL-36 activity mediates dominant activation of CD4+ T cells as the main source of IL-17 in GPP. This distinguishes GPP from chronic plaque psoriasis. Psoriasis has a similar genetic architecture to ankylosing spondylitis and Behçet's disease, where HLA-B*27 and HLA-B*51 mediate disease risk in epistasis with ERAP1 variants. In both psoriasis and Behçet's disease, we find a strong lesional infiltration of CD8+ T cells producing IL-17, indicating similar pathogenic pathways. We further searched the evolutionary origin of these HLA-class I risk alleles. We find that HLA-C*06:02, HLA-B*27 and HLA-B*51 as well as several pathogenic ERAP1 haplotypes introgressed from Denisovan and Neanderthal genomes. Our findings suggest that the protective property of the three HLA- alleles against viral infections is associated with an increased risk of autoimmune reactions. The HLA-C*06:02-restricted autoimmune response against melanocytes which can be triggered by environmental antigens is thus a central pathogenetic momentum in the development of psoriasis which may have its origin in archaic hominins.

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