Genetic variation in IRF4 expression modulates growth characteristics, tyrosinase expression and interferon-gamma response in melanocytic cells

Yash Chhabra, Hilary X.L. Yong, Mitchell Fane, Arish Soogrim, Wen Lim, Dayana Nur Mahiuddin, Reuben S.Q. Kim, Melinda Ashcroft, Scott A. Beatson, Stephen A. Ainger, Darren J. Smit, Kasturee Jagirdar, Graeme J. Walker, Richard A. Sturm, Aaron G. Smith

Research output: Contribution to journalArticlepeer-review

22 Scopus citations

Abstract

A SNP within intron4 of the interferon regulatory factor4 (IRF4) gene, rs12203592*C/T, has been independently associated with pigmentation and age-specific effects on naevus count in European-derived populations. We have characterized the cis-regulatory activity of this intronic region and using human foreskin-derived melanoblast strains, we have explored the correlation between IRF4 rs12203592 homozygous C/C and T/T genotypes with TYR enzyme activity, supporting its association with pigmentation traits. Further, higher IRF4 protein levels directed by the rs12203592*C allele were associated with increased basal proliferation but decreased cell viability following UVR, an etiological factor in melanoma development. Since UVR, and accompanying IFNγ-mediated inflammatory response, is associated with melanomagenesis, we evaluated its effects in the context of IRF4 status. Manipulation of IRF4 levels followed by IFNγ treatment revealed a subset of chemokines and immuno-evasive molecules that are sensitive to IRF4 expression level and genotype including CTLA4 and PD-L1.

Original languageEnglish
Pages (from-to)51-63
Number of pages13
JournalPigment Cell and Melanoma Research
Volume31
Issue number1
DOIs
StatePublished - Jan 2018

Keywords

  • IRF4
  • MITF
  • UVR response
  • interferon response
  • melanocyte
  • melanoma
  • tyrosinase

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