Data in Brief (Dec 2015)

NFATc1 regulates the transcription of DNA damage-induced apoptosis suppressor

  • Joo-Young Im,
  • Kang-Woo Lee,
  • Kyoung-Jae Won,
  • Bo-Kyung Kim,
  • Hyun Seung Ban,
  • Sung-Hoon Yoon,
  • Young-Ju Lee,
  • Young-Joo Kim,
  • Kyung-Bin Song,
  • Misun Won

DOI
https://doi.org/10.1016/j.dib.2015.11.011
Journal volume & issue
Vol. 5, no. C
pp. 975 – 980

Abstract

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DNA damage induced apoptosis suppressor (DDIAS), or human Noxin (hNoxin), is strongly expressed in lung cancers. DDIAS knockdown induced apoptosis in non-small cell lung carcinoma A549 cells in response to DNA damage, indicating DDIAS as a potential therapeutic target in lung cancer. To understand the transcriptional regulation of DDIAS, we determined the transcription start site, promoter region, and transcription factor. We found that DDIAS transcription begins at nucleotide 212 upstream of the DDIAS translation start site. We cloned the DDIAS promoter region and identified NFAT2 as a major transcription factor (Im et al., 2016 [1]). We demonstrated that NFATc1 regulates DDIAS expression in both pancreatic cancer Panc-1 cells and lung cancer cells.

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