Pharmacological Research - Modern Chinese Medicine (Sep 2023)

Devil's club Falcarinol inhibits human glioblastoma cell proliferation and tumor progression in xenografts

  • Susan S.C. Cheung,
  • Djamel Khelifi,
  • Zhuo-Shun Yang,
  • David Hasman,
  • Long-Jun Dai,
  • Jin-Xin Xin,
  • Bin Wang,
  • Joseph Tai

DOI
https://doi.org/10.1016/j.prmcm.2023.100271
Journal volume & issue
Vol. 8
p. 100271

Abstract

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Background: Effective treatment for human glioblastoma is lacking and a novel effective therapeutic agent is urgently needed. It is known that falcarinol-type polyacetylenes (FC-type PAs) are bioactive ingredients in ginseng and other plants from the Araliaceae family. Our earlier study showed that polyacetylene Falcarinol (FC), 1,2-dihydrofalcarinol (FCH) and 3-acetoxyfalcarinol (FCA) are potent proliferation inhibitors of human pancreatic ductal cancer cell lines. Methods: In this study we evaluated the bioactivities of these synthetic FC-type polyacetylenes (FC-type PAs) on human glioblastoma DBTRG-05MG cell line with cell viability, cell proliferation, cell migration, wound healing and clonogenic assays. We further evaluated synthetic FC on inhibition of DBTRG tumor bearing NOD-Prkdcem26Il2rgem26/Nju (NCG) mice. Results: FC dose dependently shifted DBTRG-05MG cells toward apoptosis as well as necrosis. FC and FCA, but not FCH, at near IC50 concentration inhibited colony formation in a 3-week clonogenic assay. Twice weekly intra-peritoneal injection of FC at 10 mg/kg significantly reduced tumor growth and tumor size compared to untreated control animals. Conclusions: Synthetic FC inhibits human glioblastoma cancer cell proliferation in vitro and in vivo. The availability of synthetic FC and other FC-type PAs in sufficient quantity and consistent quality would facilitate and expedite further research leading to potential clinical applications.

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