AI Article Synopsis

  • This study explores the role of ferroptosis-related genes (FRGs) in psoriasis, finding 199 differentially expressed FRGs that are linked to immune response and autophagy.* -
  • It identifies 11 key marker genes that may play significant roles in psoriasis by influencing various pathways, including the cell cycle and immune system responses.* -
  • The research also highlights potential therapeutic targets with 37 drugs that act on the identified marker genes, emphasizing the need for further studies to confirm these findings for clinical diagnosis of psoriasis.*

Article Abstract

Introduction: Ferroptosis is associated with multiple pathophysiological processes. Inhibition of ferroptosis has received much concern for some diseases. Nonetheless, there is no study comprehensively illustrating functions of ferroptosis-related genes (FRGs) in psoriasis.

Methods: In this study, FRGs together with psoriasis-associated data were obtained in Ferroptosis Database (FerrDb) and gene expression omnibus (GEO) database separately. This work identified altogether 199 psoriasis-associated DE-FRGs, and they were tightly associated with immunity and autophagy modulation. Thereafter, the present study utilized SVM-RFE and LASSO algorithms to identify NR5A2, CISD1, GCLC, PRKAA2, TRIB2, ABCC5, ACSF2, TIMM9, DCAF7, PEBP1, and MDM2 from those 199 DE-FRGs to be marker genes. As revealed by later functional annotation, the marker genes possibly had important effects on psoriasis through being involved in diverse psoriasis pathogenesis-related pathways such as cell cycle, toll-like receptor (TLR), chemokine, and nod-like receptor (NLR) pathways. Moreover, altogether 37 drugs that targeted 11 marker genes were acquired. Besides, based on CIBERSORT analysis, alterations of immune microenvironment in psoriasis cases were possibly associated with PRKAA2, PEBP1, CISD1, and ACSF2.

Discussion: Taken together, this work established the diagnostic potency and shed more lights on psoriasis-related mechanism. More investigations are warranted to validate its value in diagnosing psoriasis before it is applied in clinic.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9846571PMC
http://dx.doi.org/10.3389/fimmu.2022.1104462DOI Listing

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