AI Article Synopsis

  • The study explores how microRNAs (miRNAs) influence keratinocyte differentiation and skin diseases, focusing on the roles of mRNA and miRNA during this process.
  • Researchers found that during keratinocyte differentiation, there was a significant increase in upregulated miRNAs (76%), whereas mRNAs had a balanced up and down regulation (49% and 51%).
  • Notably, miR-155 was identified as a key inhibitor of keratinocyte differentiation and was found to be upregulated in psoriatic skin, suggesting it could be a potential target for psoriasis treatment.

Article Abstract

The role of microRNAs (miRNAs) during keratinocyte (KC) differentiation and in skin diseases with epidermal phenotypes has attracted strong interest over the past few years. However, combined mRNA and miRNA expression analyses to elucidate the intricate mRNA-miRNA networks of KCs at different stages of differentiation have not been performed yet. In the present study, we investigated the dynamics of miRNA and mRNA expression during KC differentiation in vitro and in normal and psoriatic epidermis. While we identified comparable numbers of up- and downregulated mRNAs (49% and 51%, respectively), miRNAs were predominantly upregulated (76% vs 24%) during KC differentiation. Further bioinformatics analyses suggested an important inhibitory role for miR-155 in KC differentiation, as it was repressed during KC differentiation in normal skin but strongly upregulated in the epidermis of psoriatic skin lesions. Mimicking the inflammatory milieu of psoriatic skin in vitro, we could show that the pro-inflammatory cytokines IL17, IL1β and INFγ synergistically upregulated miR-155 expression in KCs. Forced over-expression of miR-155 in human in vitro skin models specifically reduced the expression of loricrin (LOR) in KCs, indicating that miR-155 interferes with the establishment of a normal epidermal barrier. Together, our data indicate that downregulation of miR-155 during KC differentiation is a crucial step for epidermal barrier formation. Furthermore, its strong upregulation in psoriatic lesions suggests a contributing role of miR-155 in the altered keratinocyte differentiation observed in psoriasis. Therefore, miR-155 represents as a potential target for treating psoriatic skin lesions.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7731132PMC
http://dx.doi.org/10.3390/ijms21239288DOI Listing

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