Psoriatic arthritis subtypes are phenocopied in humanized mice
Christopher T. Ritchlin, … , Francisco Tausk, Maria de la Luz Garcia-Hernandez
Christopher T. Ritchlin, … , Francisco Tausk, Maria de la Luz Garcia-Hernandez
Published August 8, 2024
Citation Information: JCI Insight. 2024;9(15):e178213. https://doi.org/10.1172/jci.insight.178213.
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Research Article Dermatology Inflammation

Psoriatic arthritis subtypes are phenocopied in humanized mice

Abstract

Psoriatic arthritis (PsA) is a complex inflammatory disease that challenges diagnosis and complicates the rational selection of effective therapies. Although T cells are considered active effectors in psoriasis and PsA, the role of CD8+ T cells in pathogenesis is not well understood. We selected the humanized mouse model NSG-SGM3 transgenic strain to examine psoriasis and PsA endotypes. Injection of PBMCs and sera from patients with psoriasis and PsA generated parallel skin and joint phenotypes in the recipient mouse. The transfer of human circulating memory T cells was followed by migration and accumulation in the skin and synovia of these immunodeficient mice. Unexpectedly, immunoglobulins were required for recapitulation of the clinical phenotype of psoriasiform lesions and PsA domains (dactylitis, enthesitis, bone erosion). Human CD8+ T cells expressing T-bet, IL-32 and CXCL14 were detected by spatial transcriptomics in murine synovia and by immunofluorescence in the human PsA synovia. Importantly, depletion of human CD8+ T cells prevented skin and synovial inflammation in mice humanized with PsA peripheral blood cells. The humanized model of psoriasis and PsA represents a valid platform for accelerating the understanding of disease pathogenesis, improving the design of personalized therapies, and revealing psoriatic disease targets.

Authors

Christopher T. Ritchlin, Javier Rangel-Moreno, Delaney Martino, Brian Isett, Ananta Paine, Soumyaroop Bhattacharya, Jeffrey Fox, Ernest M. Meyer, Riyue Bao, Tullia Bruno, Francisco Tausk, Maria de la Luz Garcia-Hernandez

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Figure 6

Immunoglobulins, but not complement, are essential to induce psoriasiform lesions and arthritis in hu-PsA mice.

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Immunoglobulins, but not complement, are essential to induce psoriasifor...
(AC) Representative photographs and histology of skin from NSG-SGM3 mice injected with immunoglobulins, complete or heat-inactivated (HI) sera from a patient with PsA show (A) psoriasiform lesions, (B) increased epidermal thickness, and (C) substantial accumulation of proliferating CD3 T cells (CD3, red; Ki67, white) compared with mice injected with low-molecular-weight proteins or HC sera. (DF) Morphometric analysis of (D) epidermal thickness and (E) the number of proliferative T cells or (F) type 1 T cells. The graphs show the average ± SD of 4 mice injected with sera and PBMCs from the same patient. Significance was calculated with 2-way ANOVA and Tukey’s multiple comparison test. *P ≤ 0.05; **P ≤ 0.005. (G and H) Representative cropped (original magnification, ×200) images from a 6 × 4 mosaic of hu-PsA mice generated with complete sera, HI sera, or immunoglobulins isolated from PsA sera show (G) bigger pannus areas and (H) abundant proliferative T cells compared with mice injected with low-molecular-weight proteins from a patient with PsA sera or HC sera. Scale bar: 1,000 μm (bright-field images); 200 μm (IF images).