Frontiers in Immunology (Feb 2024)

Spatial transcriptomics reveals altered lipid metabolism and inflammation-related gene expression of sebaceous glands in psoriasis and atopic dermatitis

  • Peter Seiringer,
  • Peter Seiringer,
  • Christina Hillig,
  • Alexander Schäbitz,
  • Alexander Schäbitz,
  • Manja Jargosch,
  • Manja Jargosch,
  • Anna Caroline Pilz,
  • Anna Caroline Pilz,
  • Stefanie Eyerich,
  • Andrea Szegedi,
  • Andrea Szegedi,
  • Michaela Sochorová,
  • Michaela Sochorová,
  • Florian Gruber,
  • Florian Gruber,
  • Christos C. Zouboulis,
  • Tilo Biedermann,
  • Michael P. Menden,
  • Michael P. Menden,
  • Kilian Eyerich,
  • Kilian Eyerich,
  • Daniel Törőcsik,
  • Daniel Törőcsik

DOI
https://doi.org/10.3389/fimmu.2024.1334844
Journal volume & issue
Vol. 15

Abstract

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Sebaceous glands drive acne, however, their role in other inflammatory skin diseases remains unclear. To shed light on their potential contribution to disease development, we investigated the spatial transcriptome of sebaceous glands in psoriasis and atopic dermatitis patients across lesional and non-lesional human skin samples. Both atopic dermatitis and psoriasis sebaceous glands expressed genes encoding key proteins for lipid metabolism and transport such as ALOX15B, APOC1, FABP7, FADS1/2, FASN, PPARG, and RARRES1. Also, inflammation-related SAA1 was identified as a common spatially variable gene. In atopic dermatitis, genes mainly related to lipid metabolism (e.g. ACAD8, FADS6, or EBP) as well as disease-specific genes, i.e., Th2 inflammation-related lipid-regulating HSD3B1 were differentially expressed. On the contrary, in psoriasis, more inflammation-related spatially variable genes (e.g. SERPINF1, FKBP5, IFIT1/3, DDX58) were identified. Other psoriasis-specific enriched pathways included lipid metabolism (e.g. ACOT4, S1PR3), keratinization (e.g. LCE5A, KRT5/7/16), neutrophil degranulation, and antimicrobial peptides (e.g. LTF, DEFB4A, S100A7-9). In conclusion, our results show that sebaceous glands contribute to skin homeostasis with a cell type-specific lipid metabolism, which is influenced by the inflammatory microenvironment. These findings further support that sebaceous glands are not bystanders in inflammatory skin diseases, but can actively and differentially modulate inflammation in a disease-specific manner.

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