Journal of Translational Medicine (Aug 2012)

<it>IRF5</it> gene polymorphisms in melanoma

  • Uccellini Lorenzo,
  • De Giorgi Valeria,
  • Zhao Yingdong,
  • Tumaini Barbara,
  • Erdenebileg Narnygerel,
  • Dudley Mark E,
  • Tomei Sara,
  • Bedognetti Davide,
  • Ascierto Maria,
  • Liu Qiuzhen,
  • Simon Richard,
  • Kottyan Leah,
  • Kaufman Kenneth M,
  • Harley John B,
  • Wang Ena,
  • Rosenberg Steven A,
  • Marincola Francesco M

DOI
https://doi.org/10.1186/1479-5876-10-170
Journal volume & issue
Vol. 10, no. 1
p. 170

Abstract

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Abstract Background Interferon regulatory factor (IRF)-5 is a transcription factor involved in type I interferon signaling whose germ line variants have been associated with autoimmune pathogenesis. Since relationships have been observed between development of autoimmunity and responsiveness of melanoma to several types of immunotherapy, we tested whether polymorphisms of IRF5 are associated with responsiveness of melanoma to adoptive therapy with tumor infiltrating lymphocytes (TILs). Methods 140 TILs were genotyped for four single nucleotide polymorphisms (rs10954213, rs11770589, rs6953165, rs2004640) and one insertion-deletion in the IRF5 gene by sequencing. Gene-expression profile of the TILs, 112 parental melanoma metastases (MM) and 9 cell lines derived from some metastases were assessed by Affymetrix Human Gene ST 1.0 array. Results Lack of A allele in rs10954213 (G > A) was associated with non-response (p in vitro between cell lines carrying or not the A allele could be applied to the transcriptional profile of 112 melanoma metastases to predict their responsiveness to therapy, suggesting that IRF5 genotype may influence immune responsiveness by affecting the intrinsic biology of melanoma. Conclusions This study is the first to analyze associations between melanoma immune responsiveness and IRF5 polymorphism. The results support a common genetic basis which may underline the development of autoimmunity and melanoma immune responsiveness.