PLoS ONE (Jan 2016)

The Curcumin Analog C-150, Influencing NF-κB, UPR and Akt/Notch Pathways Has Potent Anticancer Activity In Vitro and In Vivo.

  • László Hackler,
  • Béla Ózsvári,
  • Márió Gyuris,
  • Péter Sipos,
  • Gabriella Fábián,
  • Eszter Molnár,
  • Annamária Marton,
  • Nóra Faragó,
  • József Mihály,
  • Lajos István Nagy,
  • Tibor Szénási,
  • Andrea Diron,
  • Árpád Párducz,
  • Iván Kanizsai,
  • László G Puskás

DOI
https://doi.org/10.1371/journal.pone.0149832
Journal volume & issue
Vol. 11, no. 3
p. e0149832

Abstract

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C-150 a Mannich-type curcumin derivative, exhibited pronounced cytotoxic effects against eight glioma cell lines at micromolar concentrations. Inhibition of cell proliferation by C-150 was mediated by affecting multiple targets as confirmed at transcription and protein level. C-150 effectively reduced the transcription activation of NFkB, inhibited PKC-alpha which are constitutively over-expressed in glioblastoma. The effects of C-150 on the Akt/ Notch signaling were also demonstrated in a Drosophila tumorigenesis model. C-150 reduced the number of tumors in Drosophila with similar efficacy to mitoxantrone. In an in vivo orthotopic glioma model, C-150 significantly increased the median survival of treated nude rats compared to control animals. The multi-target action of C-150, and its preliminary in vivo efficacy would render this curcumin analogue as a potent clinical candidate against glioblastoma.