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    • Psoriasis
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    • Afonina, Inna S2
    • van Nuffel, Elien2
    • Hailfinger, Stephan1
    • Schmitt, Anja1
    • Schulze-Osthoff, Klaus1

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    • Journal of Investigative Dermatology2

    Keyword

    • B-cell lymphoma/leukemia 101
    • BCL101
    • CARD-containing MAGUK protein1
    • CARD141
    • CARMA1
    • caspase recruitment domain-containing protein 141
    • CC1
    • coiled coil1
    • MAGUK1
    • MALT11
    • membrane-associated guanylate kinase1
    • mucosa-associated lymphoid tissue lymphoma translocation protein 11
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    • Commentary
      Open Archive

      Psoriasis Plays a Wild CARD

      Journal of Investigative Dermatology
      Vol. 138Issue 9p1903–1905Published in issue: September, 2018
      • Elien Van Nuffel
      • Inna S. Afonina
      • Rudi Beyaert
      Cited in Scopus: 2
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        Rare autosomal mutations in CARD14 have previously been linked to psoriasis susceptibility in humans, but their pathogenic role had not been shown. Mellett et al. generated mice harboring the patient-derived gain-of-function Card14ΔE138 mutation and showed that hyperactivation of CARD14 alone is sufficient to induce immunopathogenic mechanisms that are responsible for psoriasis, which is driven by the IL-17/IL-23 axis.
        Psoriasis Plays a Wild CARD
      • Review
        Open Archive

        CARD14-Mediated Activation of Paracaspase MALT1 in Keratinocytes: Implications for Psoriasis

        Journal of Investigative Dermatology
        Vol. 137Issue 3p569–575Published online: December 8, 2016
        • Elien Van Nuffel
        • Anja Schmitt
        • Inna S. Afonina
        • Klaus Schulze-Osthoff
        • Rudi Beyaert
        • Stephan Hailfinger
        Cited in Scopus: 28
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          Mutations in caspase recruitment domain-containing protein 14 (CARD14) have been linked to susceptibility to psoriasis. CARD14 is an intracellular scaffold protein that regulates proinflammatory gene expression. Recent studies have offered novel insights into the mechanisms of CARD14-mediated signaling in keratinocytes and the molecular impact of psoriasis-associated CARD14 mutations. CARD14 forms a signaling complex with BCL10 and the paracaspase MALT1, and this process is enhanced upon pathogenic CARD14 mutation, culminating in the activation of MALT1 protease activity and psoriasis-associated gene expression.
          CARD14-Mediated Activation of Paracaspase MALT1 in Keratinocytes: Implications for Psoriasis
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