PLoS ONE (Jan 2012)

An anilinoquinazoline derivative inhibits tumor growth through interaction with hCAP-G2, a subunit of condensin II.

  • Hirokazu Shiheido,
  • Yuhei Naito,
  • Hironobu Kimura,
  • Hiroaki Genma,
  • Hideaki Takashima,
  • Mayuko Tokunaga,
  • Takao Ono,
  • Tatsuya Hirano,
  • Wenlin Du,
  • Taketo Yamada,
  • Nobuhide Doi,
  • Shiro Iijima,
  • Yutaka Hattori,
  • Hiroshi Yanagawa

DOI
https://doi.org/10.1371/journal.pone.0044889
Journal volume & issue
Vol. 7, no. 9
p. e44889

Abstract

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We screened 46 novel anilinoquinazoline derivatives for activity to inhibit proliferation of a panel of human cancer cell lines. Among them, Q15 showed potent in vitro growth-inhibitory activity towards cancer cell lines derived from colorectal cancer, lung cancer and multiple myeloma. It also showed antitumor activity towards multiple myeloma KMS34 tumor xenografts in lcr/scid mice in vivo. Unlike the known anilinoquinazoline derivative gefitinib, Q15 did not inhibit cytokine-mediated intracellular tyrosine phosphorylation. Using our mRNA display technology, we identified hCAP-G2, a subunit of condensin II complex, which is regarded as a key player in mitotic chromosome condensation, as a Q15 binding partner. Immunofluorescence study indicated that Q15 compromises normal segregation of chromosomes, and therefore might induce apoptosis. Thus, our results indicate that hCAP-G2 is a novel therapeutic target for development of drugs active against currently intractable neoplasms.