Biochemistry and Biophysics Reports (Mar 2017)

LSD1/KDM1 isoform LSD1+8a contributes to neural differentiation in small cell lung cancer

  • Takanobu Jotatsu,
  • Shigehiro Yagishita,
  • Ken Tajima,
  • Fumiyuki Takahashi,
  • Kaoru Mogushi,
  • Moulid Hidayat,
  • Aditya Wirawan,
  • Ryo Ko,
  • Ryota Kanemaru,
  • Naoko Shimada,
  • Keiko Mitani,
  • Tsuyoshi Saito,
  • Kazuya Takamochi,
  • Kenji Suzuki,
  • Shinji Kohsaka,
  • Shinya Kojima,
  • Hiroshi Mukae,
  • Kazuhiro Yatera,
  • Kazuhisa Takahashi

DOI
https://doi.org/10.1016/j.bbrep.2016.11.015
Journal volume & issue
Vol. 9, no. C
pp. 86 – 94

Abstract

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Small cell lung cancer (SCLC) is an aggressive neuroendocrine tumor characterized by rapid progression. The mechanisms that lead to a shift from initial therapeutic sensitivity to ultimate therapeutic resistance are poorly understood. Although the SCLC genomic landscape led to the discovery of promising agents targeting genetic alterations that were already under investigation, results have been disappointing. Achievements in targeted therapeutics have not been observed for over 30 years. Therefore, the underlying disease biology and novel targets urgently require a better understanding. Epigenetic regulation is deeply involved in the cellular plasticity that could shift tumor cells to the malignant phenotype. We have focused on a histone modifier, LSD1, that is overexpressed in SCLC and is a potent therapeutic target. Interestingly, the LSD1 splice variant LSD1+8a, the expression of which has been reported to be restricted to neural tissue, was detected and was involved in the expression of neuroendocrine marker genes in SCLC cell lines. Cells with high expression of LSD1+8a were resistant to CDDP and LSD1 inhibitor. Moreover, suppression of LSD1+8a inhibited cell proliferation, indicating that LSD1+8a could play a critical role in SCLC. These findings suggest that LSD1+8a should be considered a novel therapeutic target in SCLC.

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