Th17 Cells Carrying TCR Recognizing Epidermal Autoantigen Induce Psoriasis-like Skin Inflammation

Nishimoto, Shuhei; Kotani, Hitoshi; Tsuruta, Sanae; Shimizu, N; Ito, Minako; Shichita, Takashi; Morita, Rimpei; Takahashi, Hayato; Amagai, Masayuki; Yoshimura, Akihiko

doi:10.4049/jimmunol.1300348

Cited by 40 publications

(23 citation statements)

References 39 publications

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“…This strengthens the concept that not only ACD, but also psoriasis is driven primarily by immune responses to specific stimuli [6]. Recent evidence argue for epidermal antigens such as desmoglein 3 as potential trigger of a psoriatic T cell response [26]. While in line with the literature, in nickel-induced ACD a Th2 and a cytotoxic immune response mediated by CD8+ T cells was more frequent than in psoriasis [18], psoriasis lesions were infiltrated by a higher number of IL-17+ immune cells [27].…”

Section: Discussionsupporting

confidence: 75%

Allergic Contact Dermatitis in Psoriasis Patients: Typical, Delayed, and Non-Interacting

et al. 2014

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Psoriasis is characterized by an apoptosis-resistant and metabolic active epidermis, while a hallmark for allergic contact dermatitis (ACD) is T cell-induced keratinocyte apoptosis. Here, we induced ACD reactions in psoriasis patients sensitized to nickel (n = 14) to investigate underlying mechanisms of psoriasis and ACD simultaneously. All patients developed a clinically and histologically typical dermatitis upon nickel challenge even in close proximity to pre-existing psoriasis plaques. However, the ACD reaction was delayed as compared to non-psoriatic patients, with a maximum intensity after 7 days. Whole genome expression analysis revealed alterations in numerous pathways related to metabolism and proliferation in non-involved skin of psoriasis patients as compared to non-psoriatic individuals, indicating that even in clinically non-involved skin of psoriasis patients molecular events opposing contact dermatitis may occur. Immunohistochemical comparison of ACD reactions as well as in vitro secretion analysis of lesional T cells showed a higher Th17 and neutrophilic migration as well as epidermal proliferation in psoriasis, while ACD reactions were dominated by cytotoxic CD8+ T cells and a Th2 signature. Based on these findings, we hypothesized an ACD reaction directly on top of a pre-existing psoriasis plaque might influence the clinical course of psoriasis. We observed a strong clinical inflammation with a mixed psoriasis and eczema phenotype in histology. Surprisingly, the initial psoriasis plaque was unaltered after self-limitation of the ACD reaction. We conclude that sensitized psoriasis patients develop a typical, but delayed ACD reaction which might be relevant for patch test evaluation in clinical practice. Psoriasis and ACD are driven by distinct and independent immune mechanisms.

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Section: Discussionsupporting

confidence: 75%

Allergic Contact Dermatitis in Psoriasis Patients: Typical, Delayed, and Non-Interacting

et al. 2014

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“…This mechanism may also play a role in other autoimmune diseases because high levels of IL-17 similar to that detected in our patients have been described in SLE, 24,28 RA, 29,30 and psoriasis. [31][32][33] Moreover, decreased Fas function has been also detected in patients displaying autoimmune diseases different from ALPS and DALD. [34][35][36] The antiapoptotic effect of IL-17s may be partly due to modulation of cFLIP expression since exposure to IL-17A substantially upmodulated cFLIP S and downmodulated cFLIP L in Fas-stimulated T cells.…”

Section: Discussionmentioning

confidence: 99%

IL-17 protects T cells from apoptosis and contributes to development of ALPS-like phenotypes

Boggio

Clemente

Mondino

et al. 2014

Blood

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“…In fact, anti-TNF is a mainstay of therapy for psoriasis, and anti-IL-17A therapy was recently approved as a first-line systemic treatment (10,11). While the involvement of peptide-reactive T cells has been well defined (12)(13)(14)(15), the role of lipid-reactive T cells in psoriasis remains largely unknown. Since psoriasis and cardiovascular disease are correlated with hyperlipidemia and recent studies have identified CD1-restricted self-lipid-reactive T cells in the blood or skin of humans (16)(17)(18)(19), we developed a new mouse model for the study of human CD1-restricted T cell responses to self-lipids in vivo.…”

Section: Introductionmentioning

confidence: 99%

CD1b-autoreactive T cells contribute to hyperlipidemia-induced skin inflammation in mice

Bagchi¹,

Hé²,

Zhao³

et al. 2017

Journal of Clinical Investigation

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Th17 Cells Carrying TCR Recognizing Epidermal Autoantigen Induce Psoriasis-like Skin Inflammation

Cited by 40 publications

References 39 publications

Allergic Contact Dermatitis in Psoriasis Patients: Typical, Delayed, and Non-Interacting

Allergic Contact Dermatitis in Psoriasis Patients: Typical, Delayed, and Non-Interacting

IL-17 protects T cells from apoptosis and contributes to development of ALPS-like phenotypes

CD1b-autoreactive T cells contribute to hyperlipidemia-induced skin inflammation in mice

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