The psoriasis-associated IL-17A induces and cooperates with IL-36 cytokines to control keratinocyte differentiation and function

Pfaff, Carolina M.; Marquardt, Yvonne; Fietkau, Katharina; Baron, Jens Malte; Lüscher, Bernhard

doi:10.1038/s41598-017-15892-7

Cited by 107 publications

(81 citation statements)

References 55 publications

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“…Our research and previous studies showed that IL‐17A directly suppressed profilaggrin/FLG protein production by downregulating its mRNA expression ( FLG ) (Fig. e) . As a result, IL‐17A decreased the keratohyalin granules in the epidermal construct and induced a thin granular layer in a 3‐D epidermis model, whereas IL‐17C did not affect the structure (Fig.…”

Section: Discussionsupporting

confidence: 63%

Interleukin‐17A suppresses granular layer formation in a 3‐D human epidermis model through regulation of terminal differentiation genes

Sato

Fujita

Imafuku

2020

The Journal of Dermatology

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Immunotherapies targeting interleukin (IL)‐17 greatly improve plaque psoriasis. Most previous studies on IL‐17 focused on the T‐helper (Th)17 immune response, but investigation of the effects of IL‐17A on psoriatic epidermal structure are limited. Using an in vitro 3‐D human epidermis model, we investigated the effects of IL‐17A and IL‐17C on morphological changes and gene expression. IL‐17A directly suppressed the formation of the granular layer, whereas IL‐17C did not. IL‐17A significantly downregulated the gene expression of profilaggrin (FLG), which is a major component of keratohyalin granules in the granular layer. Global gene expression analysis of this 3‐D epidermis model showed that both IL‐17A and IL‐17C upregulated S100A7A and type 1 interferon‐related genes including MX1, IFI44L, XAF1 and IFIT1. However, only IL‐17A directly downregulated keratinocyte differentiation‐related and cornified envelope‐related genes including FLG, LOR, C1ORF68, LCE1E, LCE1B, KRT10, CST6 and RPTN. In conclusion, IL‐17A, a systemic inflammatory cytokine, affected keratinization in our 3‐D epidermis model. In contrast, IL‐17C, a locally produced cytokine, did not have strong effects on keratinization. Targeting IL‐17A does not only reduce inflammation but it may also directly affect epidermal differentiation in psoriasis.

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Section: Discussionsupporting

confidence: 63%

Interleukin‐17A suppresses granular layer formation in a 3‐D human epidermis model through regulation of terminal differentiation genes

Sato

Fujita

Imafuku

2020

The Journal of Dermatology

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“…Neutrophils in active psoriatic lesions are the largest fraction of infiltrating cells containing IL‐17, which is preformed by T‐helper 17 cells (or possibly derived from neutrophils themselves) and also highly expressed in the lesion of GPP . Previous studies indicated that psoriasis‐associated IL‐17A deregulates gene expression of IL‐36 cytokine family members in keratinocytes, which are essential for the keratinocyte feedback control, the cross‐talk between keratinocytes and neutrophils, and the influx of neutrophils into psoriatic lesions including GPP . The proteases released from the stimulated neutrophils may further activate the IL‐36 cytokines by proteolytic processing .…”

Section: Discussionmentioning

confidence: 99%

“…The proteases released from the stimulated neutrophils may further activate the IL‐36 cytokines by proteolytic processing . The DITRA due to homozygous mutations in IL36RN may enhance the inflammatory responses induced by IL‐36 cytokines, which synergize with IL‐17A and amplify the vicious cycle between keratinocytes and neutrophils in GPP …”

Section: Discussionmentioning

confidence: 99%

Successful treatment of refractory juvenile generalized pustular psoriasis with secukinumab monotherapy: A case report and review of published work

Tsai

2018

The Journal of Dermatology

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Juvenile generalized pustular psoriasis (GPP) is rare and often resistant to conventional systemic therapy such as methotrexate, retinoic acid and cyclosporin A. GPP can be induced by deficiency of interleukin (IL)-36 receptor antagonist (DITRA). No standardized guidelines are available for juvenile GPP or DITRA, and a uniformly safe and effective biologic agent has not been identified. However, multiple biologics approved for use in plaque-type psoriasis have also been used in GPP. Herein, we report a case of a 6-year-old Taiwanese boy with GPP and homozygous mutation at c.115+6T>C within the IL-36 receptor antagonist (IL36RN) gene, who was treated successfully with secukinumab after failure of prior methotrexate, acitretin, cyclosporin A, etanercept and adalimumab. Similar to two previously reported non-adult cases of GPP successfully treated with secukinumab, our case also demonstrated a history of repeated treatment failures with several conventional oral systemic agents and biologics. Different from these two cases, however, ours is the first of juvenile GPP successfully treated with secukinumab monotherapy, without using other systemic agent concurrently during the use of secukinumab.

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“…IL‐36γ is a potent inflammatory member of the IL‐1 family, produced by keratinocytes in response to multiple stimuli including cell damage . The role of IL‐36γ in psoriasis pathogenesis is increasingly recognized .…”

Section: Introductionmentioning

confidence: 99%

IL‐17A synergistically enhances TLR3‐mediated IL‐36γ production by keratinocytes: A potential role in injury‐amplified psoriatic inflammation

Liu

et al. 2019

Experimental Dermatology

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Skin injury can trigger formation of new lesions in psoriasis (Koebner phenomenon). The mechanisms through which injury exacerbates psoriasis are unclear. During wound repair, epidermal keratinocytes are activated and produce abundant IL‐36γ, further promoting the skin inflammation. IL‐17A is the cornerstone cytokine in the pathogenesis of psoriasis. We sought to investigate the effects of IL‐17A on injury‐induced keratinocyte activation and IL‐36γ production. Here, we demonstrated that dsRNA released from necrotic keratinocytes induced the expression of IL‐36γ. Silencing of TLR3 by siRNA decreased the IL‐36γ induction by necrotic keratinocyte supernatant. Co‐stimulation with dsRNA and IL‐17A synergistically increased the expression of IL‐36γ and other proinflammatory mediators (CCL20, CXCL8, DEFB4 and LCN2) in keratinocytes. The synergistic effects were not dependent on TLR3 upregulation, TNF receptor signalling and mRNA stabilization. Co‐stimulation with dsRNA and IL‐17A resulted in an accumulation of IκBζ. The synergistic upregulation of IL‐36γ and proinflammatory mediators were inhibited by IκBζ siRNA. Co‐stimulation with IL‐17A and poly(I:C) markedly activated the p38 MAPK and NF‐κB pathway, compared with poly(I:C). Blockade of p38 MAPK and NF‐κB suppressed dsRNA/IL‐17A–mediated IκBζ and IL‐36γ induction. These findings demonstrated that IL‐17A synergistically enhanced the dsRNA‐mediated IL‐36γ production through a p38 MAPK‐, NF‐κB–, and IκBζ‐dependent mechanism.

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The psoriasis-associated IL-17A induces and cooperates with IL-36 cytokines to control keratinocyte differentiation and function

Cited by 107 publications

References 55 publications

Interleukin‐17A suppresses granular layer formation in a 3‐D human epidermis model through regulation of terminal differentiation genes

Interleukin‐17A suppresses granular layer formation in a 3‐D human epidermis model through regulation of terminal differentiation genes

Successful treatment of refractory juvenile generalized pustular psoriasis with secukinumab monotherapy: A case report and review of published work

IL‐17A synergistically enhances TLR3‐mediated IL‐36γ production by keratinocytes: A potential role in injury‐amplified psoriatic inflammation

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