Frontiers in Oncology (Nov 2012)

Polyamine pathway inhibition as a novel therapeutic approach to treating neuroblastoma

  • Laura Dawn Gamble,
  • Michael D Hogarty,
  • Xuenyuan eLiu,
  • David S Ziegler,
  • David S Ziegler,
  • Glenn M Marshall,
  • Glenn M Marshall,
  • Murray D Norris,
  • Michelle eHaber

DOI
https://doi.org/10.3389/fonc.2012.00162
Journal volume & issue
Vol. 2

Abstract

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Polyamines are highly regulated essential cations that are elevated in rapidly proliferating tissues, including diverse cancers. Expression analyses in neuroblastomas suggest that upregulation of polyamine pro-synthetic enzymes and downregulation of catabolic enzymes is associated with poor prognosis. Polyamine sufficiency may be required for MYCN oncogenicity in MYCN amplified neuroblastoma, and targeting polyamine homeostasis may therefore provide an attractive therapeutic approach. ODC1, an oncogenic MYCN target, is rate-limiting for polyamine synthesis, and is overexpressed in many cancers including neuroblastoma. Inhibition of ODC1 by difluoromethylornithine (DFMO) decreased tumour penetrance in TH-MYCN mice treated pre-emptively, and extended survival and synergized with chemotherapy in treating established tumours in both TH-MYCN and xenograft models. Efforts to augment DFMO activity, or otherwise maximally reduce polyamine levels, are focused on antagonizing polyamine uptake or augmenting polyamine export or catabolism. Since polyamine inhibition appears to be clinically well tolerated, these approaches, particularly when combined with chemotherapy, have great potential for improving neuroblastoma outcome in both MYCN amplified and non-MYCN amplified neuroblastomas.

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