Cell Death and Disease (Aug 2024)

Targeting miR-497-5p rescues human keratinocyte dysfunction upon skin exposure to sulfur mustard

  • Virginia Egea,
  • Karina Lutterberg,
  • Dirk Steinritz,
  • Simone Rothmiller,
  • Konrad Steinestel,
  • Jan Caca,
  • Andreas Nerlich,
  • Helmut Blum,
  • Sarah Reschke,
  • Sajjad Khani,
  • Alexander Bartelt,
  • Franz Worek,
  • Horst Thiermann,
  • Christian Weber,
  • Christian Ries

DOI
https://doi.org/10.1038/s41419-024-06974-2
Journal volume & issue
Vol. 15, no. 8
pp. 1 – 12

Abstract

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Abstract Sulfur mustard (SM) is a highly toxic chemical warfare agent. Exposure to SM results in various pathologies including skin lesions with subsequent impaired wound healing. To date, there are no effective treatments available. Here we discover a SM-triggered pathomechanism involving miR-497-5p and its target survivin which contributes to keratinocyte dysfunction. Transcriptome analysis using RNA-seq in normal human epidermal keratinocytes (NHEK) revealed that SM evoked differential expression of 1896 mRNAs and 25 miRNAs with many of these RNAs known to be involved in keratinocyte function and wound healing. We demonstrated that keratinocyte differentiation and proliferation were efficiently regulated by miRNAs induced in skin cells after exposure to SM. The inhibition of miR-497-5p counteracted SM-induced premature differentiation and stimulated proliferation of NHEK. In addition, we showed that microneedle-mediated transdermal application of lipid-nanoparticles containing miR-497-5p inhibitor restored survivin biosynthesis and cellular functionality upon exposure to SM using human skin biopsies. Our findings expand the current understanding of SM-associated molecular toxicology in keratinocytes and highlight miR-497-5p as feasible clinical target for specific skin therapy in SM-exposed patients and beyond.