Acta Pharmaceutica Sinica B (Jul 2019)

Development of the triazole-fused pyrimidine derivatives as highly potent and reversible inhibitors of histone lysine specific demethylase 1 (LSD1/KDM1A)

  • Zhonghua Li,
  • Lina Ding,
  • Zhongrui Li,
  • Zhizheng Wang,
  • Fengzhi Suo,
  • Dandan Shen,
  • Taoqian Zhao,
  • Xudong Sun,
  • Junwei Wang,
  • Ying Liu,
  • Liying Ma,
  • Bing Zhao,
  • Pengfei Geng,
  • Bin Yu,
  • Yichao Zheng,
  • Hongmin Liu

Journal volume & issue
Vol. 9, no. 4
pp. 794 – 808

Abstract

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Histone lysine specific demethylase 1 (LSD1) has been recognized as an important modulator in post-translational process in epigenetics. Dysregulation of LSD1 has been implicated in the development of various cancers. Herein, we report the discovery of the hit compound 8a (IC50 = 3.93 μmol/L) and further medicinal chemistry efforts, leading to the generation of compound 15u (IC50 = 49 nmol/L, and Ki = 16 nmol/L), which inhibited LSD1 reversibly and competitively with H3K4me2, and was selective to LSD1 over MAO-A/B. Docking studies were performed to rationalize the potency of compound 15u. Compound 15u also showed strong antiproliferative activity against four leukemia cell lines (OCL-AML3, K562, THP-1 and U937) as well as the lymphoma cell line Raji with the IC50 values of 1.79, 1.30, 0.45, 1.22 and 1.40 μmol/L, respectively. In THP-1 cell line, 15u significantly inhibited colony formation and caused remarkable morphological changes. Compound 15u induced expression of CD86 and CD11b in THP-1 cells, confirming its cellular activity and ability of inducing differentiation. The findings further indicate that targeting LSD1 is a promising strategy for AML treatment, the triazole-fused pyrimidine derivatives are new scaffolds for the development of LSD1/KDM1A inhibitors. KEY WORDS: Epigenetic regulation, Histone demethylase, LSD1, Pyrimidine-triazole, Mercapto heterocycles, Antiproliferative ability, AML treatment, Structure–activity relationships (SARs)