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CARD14E138A signalling in keratinocytes induces TNF-dependent skin and systemic inflammation

Joan Manils, Louise V. Webb, Ashleigh Howes, Julia Janzen, Stefan Boeing, A. Bowcock, Steven C. Ley

2020eLife33 citationsDOIOpen Access PDF

Abstract

To investigate how the CARD14E138A psoriasis-associated mutation induces skin inflammation, a knock-in mouse strain was generated that allows tamoxifen-induced expression of the homologous Card14E138A mutation from the endogenous mouse Card14 locus. Heterozygous expression of CARD14E138A rapidly induced skin acanthosis, immune cell infiltration and expression of psoriasis-associated pro-inflammatory genes. Homozygous expression of CARD14E138A induced more extensive skin inflammation and a severe systemic disease involving infiltration of myeloid cells in multiple organs, temperature reduction, weight loss and organ failure. This severe phenotype resembled acute exacerbations of generalised pustular psoriasis (GPP), a rare form of psoriasis that can be caused by CARD14 mutations in patients. CARD14E138A-induced skin inflammation and systemic disease were independent of adaptive immune cells, ameliorated by blocking TNF and induced by CARD14E138A signalling only in keratinocytes. These results suggest that anti-inflammatory therapies specifically targeting keratinocytes, rather than systemic biologicals, might be effective for GPP treatment early in disease progression.

Topics & Concepts

PsoriasisInflammationSystemic inflammationImmune systemImmunologyMedicinePhenotypeInfiltration (HVAC)Tumor necrosis factor alphaCancer researchBiologyGeneGeneticsThermodynamicsPhysicsPsoriasis: Treatment and PathogenesisDermatology and Skin DiseasesAsthma and respiratory diseases
CARD14E138A signalling in keratinocytes induces TNF-dependent skin and systemic inflammation | Litcius