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    • Psoriasis
    • Tsoi, Lam CRemove Tsoi, Lam C filter
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    • Original Article Clinical Research: Pathophysiology
      Open Archive

      Neutrophil Extracellular Traps Induce Human Th17 Cells: Effect of Psoriasis-Associated TRAF3IP2 Genotype

      Journal of Investigative Dermatology
      Vol. 139Issue 6p1245–1253Published online: December 5, 2018
      • Sylviane Lambert
      • Caely A. Hambro
      • Andrew Johnston
      • Philip E. Stuart
      • Lam C. Tsoi
      • Rajan P. Nair
      • and others
      Cited in Scopus: 40
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        Psoriasis lesions are rich in IL-17–producing T cells as well as neutrophils, which release webs of DNA-protein complexes known as neutrophil extracellular traps (NETs). Because we and others have observed increased NETosis in psoriatic lesions, we hypothesized that NETs contribute to increased T helper type 17 (Th17) cells in psoriasis. After stimulating peripheral blood mononuclear cells with anti-CD3/CD28 beads for 7 days, we found significantly higher percentages of CD3+CD4+IL-17+ (Th17) cells in the presence versus absence of NETs, as assessed by flow cytometry, IL-17 ELISA, and IL17A/F and RORC mRNAs.
        Neutrophil Extracellular Traps Induce Human Th17 Cells: Effect of Psoriasis-Associated TRAF3IP2 Genotype
      • Letter to the Editor
        Open Access

        A Transethnic Mendelian Randomization Study Identifies Causality of Obesity on Risk of Psoriasis

        Journal of Investigative Dermatology
        Vol. 139Issue 6p1397–1400Published online: December 5, 2018
        • Kotaro Ogawa
        • Philip E Stuart
        • Lam C. Tsoi
        • Ken Suzuki
        • Rajan P. Nair
        • Hideki Mochizuki
        • and others
        Cited in Scopus: 19
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          Psoriasis is a chronic disorder characterized by cutaneous and systemic manifestations. Epidemiological studies have reported increased comorbidity of psoriasis with numerous complex diseases such as metabolic clinical measurements (Greb et al., 2016; Naito and Imafuku, 2016). However, interpretation of the comorbidity remains controversial to date, because causal inference between correlated phenotypes is difficult when depending solely on epidemiological studies. Identification of causal inference between correlated phenotypes has significant clinical impacts, because modification of the causal phenotypes could benefit treatment of the outcome phenotypes.
          A Transethnic Mendelian Randomization Study Identifies Causality of Obesity on Risk of Psoriasis
        • Original Article Immunology/Infection
          Open Access

          Psoriasis-Associated Late Cornified Envelope (LCE) Proteins Have Antibacterial Activity

          Journal of Investigative Dermatology
          Vol. 137Issue 11p2380–2388Published online: June 17, 2017
          • Hanna Niehues
          • Lam C. Tsoi
          • Danique A. van der Krieken
          • Patrick A.M. Jansen
          • Merel A.W. Oortveld
          • Diana Rodijk-Olthuis
          • and others
          Cited in Scopus: 38
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            Terminally differentiating epidermal keratinocytes express a large number of structural and antimicrobial proteins that are involved in the physical barrier function of the stratum corneum and provide innate cutaneous host defense. Late cornified envelope (LCE) genes, located in the epidermal differentiation complex on chromosome 1, encode a family of 18 proteins of unknown function, whose expression is largely restricted to epidermis. Deletion of two members, LCE3B and LCE3C (LCE3B/C-del), is a widely-replicated psoriasis risk factor that interacts with the major psoriasis-psoriasis risk gene HLA-C*06.
            Psoriasis-Associated Late Cornified Envelope (LCE) Proteins Have Antibacterial Activity
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