AI Article Synopsis

  • Increased levels of microRNA-21 (miR-21) in psoriasis lead to a decrease in the epidermal tissue inhibitor TIMP-3, which is crucial for regulating inflammation mediated by TNFα.
  • An experimental study compared expression profiles of miR-21 and TIMP-3 in patients with medication-induced psoriasiform reactions and non-induced psoriasis.
  • Findings revealed that patients with induced psoriasis exhibited high TIMP-3 levels and low miR-21 expression, indicating distinct inflammatory mechanisms at play in paradoxical reactions compared to non-induced psoriasis.

Article Abstract

Background: Expression of microRNA-21 (miR-21) is increased in psoriasis, leading to reduced levels of epidermal tissue inhibitor of matrix metalloproteinase 3 (TIMP-3), a highly potent inhibitor of the tumor necrosis factor alpha (TNFα) sheddase TACE (TNFα-converting enzyme)/ADAM17. We described the profile of miR-21 and TIMP-3 in paradoxical psoriasiform reactions induced by anti-TNFα drugs and in a control group to elucidate the pathogenesis of this reactions.

Methods: We performed an analytic, cross-sectional, prospective, experimental case-control study. We compared our findings with those of non-induced psoriasis.

Results: We included 15 patients with a change of morphology (plaque to guttate psoriasis) and 10 patients with induced psoriasis (six palmoplantar pustulosis and four plaque psoriasis). Consecutive patients with different subtypes of non-induced, non-systemically treated psoriasis were included as a control group. We found that most cases with guttate psoriasis and with induced plaque psoriasis cases showed high expression of TIMP-3 expression and decreased or poorly increased levels of miR-21. The expression pattern was not homogeneous in the cases of induced palmoplantar pustulosis. These profiles differ from those of non-induced psoriasis.

Conclusion: We conclude that various pro-inflammatory cytokine profiles are involved in the pathogenesis of paradoxical psoriasiform reactions and non-induced psoriasis.

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Source
http://dx.doi.org/10.1111/cup.14113DOI Listing

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