Journal of Experimental & Clinical Cancer Research (Mar 2019)

A selective c-Met and Trks inhibitor Indo5 suppresses hepatocellular carcinoma growth

  • Teng Luo,
  • Shou-Guo Zhang,
  • Ling-Fei Zhu,
  • Fei-Xiang Zhang,
  • Wei Li,
  • Ke Zhao,
  • Xiao-Xue Wen,
  • Miao Yu,
  • Yi-Qun Zhan,
  • Hui Chen,
  • Chang-Hui Ge,
  • Hui-Ying Gao,
  • Lin Wang,
  • Xiao-Ming Yang,
  • Chang-Yan Li

DOI
https://doi.org/10.1186/s13046-019-1104-4
Journal volume & issue
Vol. 38, no. 1
pp. 1 – 13

Abstract

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Abstract Background Human hepatocellular carcinoma (HCC) lacks effective curative therapy and there is an urgent need to develop a novel molecular-targeted therapy for HCC. Selective tyrosine kinase inhibitors have shown promise in treating cancers including HCC. Tyrosine kinases c-Met and Trks are potential therapeutic targets of HCC and strategies to interrupt c-Met and Trks cross-signaling may result in increased effects on HCC inhibition. Methods The effects of Indo5 on c-Met and Trks activity were determined with in vitro kinase activity assay, cell-based signaling pathway activation, and kinases-driven cell transformation. The in vivo anti-tumor activity was determined with xenograft mice and liver orthotopic mice models. The co-expression of c-Met and TrkB in 180 pairs of HCC and adjacent normal tissues were detected using immunohistochemical staining. Results Indo5, a novel lead compound displayed biochemical potency against both c-Met and Trks with selectivity over 13 human kinases. Indo5 abrogated HGF-induced c-Met signaling activation and BDNF/NGF-induced Trks signal activation, c-Met or TrkB-mediated cell transformation and migration. Furthermore, Indo5 significantly decreased the growth of HCC cells in xenograft mice and improved the survival of mice with liver orthotopic tumors. In addition, co-expression of c-Met and TrkB in HCC patients was a predictor of poor prognosis, and combined inhibition of c-Met and TrkB exerted a synergistic suppressive effect on HCC. Conclusions These findings indicate that Indo5 is associated with marked suppression of c-Met and Trks co-expressing HCC, supporting its clinical development as an antitumor treatment for HCC patients with co-active c-Met and Trks signaling.

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