Biomedicine & Pharmacotherapy (Jun 2023)

Regnase-1 plays an essential role in maintaining skin immune homeostasis via regulation of chemokine expression

  • Gabsik Yang,
  • Hye Eun Lee,
  • Magdalena Trzeciak,
  • Tadeusz Pawelczyk,
  • Osamu Takeuchi,
  • Han Chang Kang,
  • Yong-Yeon Cho,
  • Hye Suk Lee,
  • Joo Young Lee

Journal volume & issue
Vol. 162
p. 114558

Abstract

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Regnase-1 is an endoribonuclease that regulates the stability of target genes. Here, we investigated whether Regnase-1 plays a regulatory role in the pathophysiology of atopic dermatitis, a chronic inflammatory skin disease. Regnase-1 levels were decreased in skin and serum of atopic dermatitis patients and mice. Regnase-1+/- mice exhibited more severe atopic dermatitis symptoms than wild-type mice in a house dust mite allergen-induced atopic dermatitis model. Regnase-1 deficiency led to the global changes in gene expression related with innate immune and inflammatory responses, in particular chemokines. The skin Regnase-1 level had an inverse relationship with chemokine expression when we analyzed samples of atopic dermatitis patients and Regnase-1-deficient mice, suggesting that potentiated chemokine production contributes to the augmented inflammation at lesion sites. Subcutaneous administration of recombinant Regnase-1 to mice significantly ameliorated atopic dermatitis-like skin inflammation with reduced chemokine production in a house dust mite-induced atopic dermatitis NC/Nga mouse model. These results indicate that Regnase-1 plays an essential role in maintaining skin immune homeostasis as a regulator of chemokine expression. Modulating Regnase-1 activity may be an efficient therapeutic strategy for treating chronic inflammatory diseases, including atopic dermatitis.

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