<scp>IL</scp>‐36 receptor antagonistic antibodies inhibit inflammatory responses in preclinical models of psoriasiform dermatitis

Su, Zhi; Paulsboe, Stephanie; Wetter, J.; Salte, K.; Kannan, A.; Mathew, Sheeba; Horowitz, Amanda; Gerstein, C.; Namovic, Marian T.; Todorović, Viktor; Seagal, Jane; Edelmayer, Rebecca M.; Viner, Michelle; Rinaldi, Lisa; Zhou, Li; Leys, Laura; Huang, Susan M.; Wang, Leyu; Sadhukhan, Ramkrishna; Honoré, Prisca; McGaraughty, Steve; Scott, Victoria E.

doi:10.1111/exd.13841

Cited by 31 publications

(42 citation statements)

References 30 publications

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“…Another severe subtype, called generalized pustular psoriasis, was found to result from an overactive IL-36 pathway (5). In agreement, neutralizing antibodies against IL-17A and IL-23 represent effective state-of-the-art therapies for the treatment of patients with psoriasis, whereas antagonizing IL-36 receptor antibodies are currently being investigated as a new therapy approach for psoriasis (6).…”

Section: Introductionmentioning

confidence: 86%

Keratinocyte-derived IκBζ drives psoriasis and associated systemic inflammation

Lorscheid¹,

Müller²,

Löffler³

et al. 2019

JCI Insight

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Section: Introductionmentioning

confidence: 86%

Keratinocyte-derived IκBζ drives psoriasis and associated systemic inflammation

Lorscheid¹,

Müller²,

Löffler³

et al. 2019

JCI Insight

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“…Hydrodynamic gene delivery is a commonly used in vivo transfection method that involves rapidly injecting a large volume of plasmid DNA into the lateral tail vein, which then forces the solution into the liver and transfects the hepatocytes. [16][17][18]24 In these studies, animals were hydrodynamically injected with IL-23 MC, causing a significant increase of IL-23 levels in both the plasma (F [14,207] = 21.55, P < 0.0001) and ear (F [14,150] = 21.21, P < 0.0001) ( Table 1). For the highest dose (3 lg), circulating plasma IL-23 levels were elevated as early as day 2 post-injection, and remained elevated throughout the 14-day study duration.…”

Section: Sustained Elevation Of Il-23 Levels In the Ear And Plasmamentioning

confidence: 99%

“…Repeated intradermal injection of IL‐23 to mice has been used as a mechanistic model that recapitulates many key features of psoriasis . These models have been useful in understanding skin inflammation associated with activation of this pathway and evaluating novel therapeutics.…”

Section: Introductionmentioning

confidence: 99%

“…6 Repeated intradermal injection of IL-23 to mice has been used as a mechanistic model that recapitulates many key features of psoriasis. [7][8][9][10][11][12][13][14] These models have been useful in understanding skin inflammation associated with activation of this pathway and evaluating novel therapeutics. An alternative means to augment endogenous IL-23 levels is to utilize hydrodynamic delivery of IL-23 minicircles (MC).…”

Section: Introductionmentioning

confidence: 99%

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Characterization of psoriasiform dermatitis induced by systemic injection of interleukin‐23 minicircles in mice

Leys

Wang

Paulsboe

et al. 2019

The Journal of Dermatology

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The interleukin (IL)‐23/IL‐17 axis plays a central role in the pathogenesis of psoriasis and is elevated in lesional psoriatic skin. Different murine models have been developed to mimic this pathophysiology each carrying specific merits and limitations. In an attempt to address some of these limitations, B10.RIII mice received a single hydrodynamic injection of IL‐23 minicircles (MC) to induce hepatic transcription and the endogenous production of IL‐23. Plasma and ear IL‐23 levels were dose‐dependently (0.3–3 μg) increased in MC injected mice and were sustained over the 14‐day study duration. Beginning on day 7 post‐injection, mice developed dose‐related ear inflammation, histologically confirmed increases in epidermal and dermal area, as well as enhanced neutrophil and macrophage content. Flow cytometry demonstrated increased levels of granulocytes, T cells and monocytes/macrophages in the ear skin, with T cells identified as the main cellular source of IL‐17A. Evaluation of mRNA and protein showed time‐dependent, increased levels of the IL‐23/IL‐17 pathway and inflammatory/microbial cytokines/chemokines in the ear which differed kinetically from circulating levels. An anti‐IL‐23p40 antibody was assessed following both prophylactic administration and administration once the disease was established. Prophylactic dosing completely prevented the development of the ear phenotype across endpoints. Treatment administration showed a dose‐related response, with a maximum inhibition of 64–94%, depending on endpoint. These data demonstrate that the IL‐23 MC model is a useful approach to study IL‐23/IL‐17‐driven skin inflammation and may facilitate preclinical assessment of novel therapies.

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“…essays on Skin Immunity, [1][2][3][4] and authoritative reviews and original research articles on (b) Cell Biology of Skin Immunity, [5][6][7] (c) Immunopathology of Atopic Dermatitis, [8][9][10][11][12] (d) Psoriasis [13][14][15] and (e) Bullous pemphigoid. [16] In addition, it covers (f) the Immunology of Wound Healing and, [17,18] and, finally, (g) Animal models in Skin Immunology Research.…”

mentioning

confidence: 99%