Clinical and Translational Medicine (Jul 2023)

HSF4/COIL complex‐dependent R‐loop mediates ultraviolet‐induced inflammatory skin injury

  • Yi‐qian Feng,
  • Heng Zhang,
  • Jing‐xia Han,
  • Bi‐jia Cui,
  • Lu‐ning Qin,
  • Lei Zhang,
  • Qing‐qing Li,
  • Xin‐ying Wu,
  • Nan‐nan Xiao,
  • Yan Zhang,
  • Ting‐ting Lin,
  • Hui‐juan Liu,
  • Tao Sun

DOI
https://doi.org/10.1002/ctm2.1336
Journal volume & issue
Vol. 13, no. 7
pp. n/a – n/a

Abstract

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Abstract Intense ultraviolet (UV) exposure can cause phototoxic reactions, such as skin inflammation, resulting in injury. UV is a direct cause of DNA damage, but the mechanisms underlying transcriptional regulation within cells after DNA damage are unclear. The bioinformatics analysis of transcriptome sequencing data from UV‐irradiated and non‐UV‐irradiated skin showed that transcription‐related proteins, such as HSF4 and COIL, mediate cellular response to UV irradiation. HSF4 and COIL can form a complex under UV irradiation, and the preference for binding target genes changed because of the presence of a large number of R‐loops in cells under UV irradiation and the ability of COIL to recognize R‐loops. The regulation of target genes was altered by the HSF4–COIL complex, and the expression of inflammation and ageing‐related genes, such as Atg7, Tfpi, and Lims1, was enhanced. A drug screen was performed for the recognition sites of COIL and R‐loop. N6‐(2‐hydroxyethyl)‐adenosine can competitively bind COIL and inhibit the binding of COIL to the R‐loop. Thus, the activation of downstream inflammation‐related genes and inflammatory skin injury was inhibited.

Keywords