PLoS ONE (Jan 2018)

Hedgehog inhibition mediates radiation sensitivity in mouse xenograft models of human esophageal adenocarcinoma.

  • Jennifer Teichman,
  • Lorin Dodbiba,
  • Henry Thai,
  • Andrew Fleet,
  • Trevor Morey,
  • Lucy Liu,
  • Madison McGregor,
  • Dangxiao Cheng,
  • Zhuo Chen,
  • Gail Darling,
  • Yonathan Brhane,
  • Yuyao Song,
  • Osvaldo Espin-Garcia,
  • Wei Xu,
  • Hala Girgis,
  • Joerg Schwock,
  • Helen MacKay,
  • Robert Bristow,
  • Laurie Ailles,
  • Geoffrey Liu

DOI
https://doi.org/10.1371/journal.pone.0194809
Journal volume & issue
Vol. 13, no. 5
p. e0194809

Abstract

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BACKGROUND:The Hedgehog (Hh) signaling pathway is active in esophageal adenocarcinoma (EAC). We used a patient-derived murine xenograft (PDX) model of EAC to evaluate tumour response to conventional treatment with radiation/chemoradiation with or without Hh inhibition. Our goal was to determine the potential radioresistance effects of Hh signaling and radiosensitization by Hh inhibitors. METHODS:PDX models were treated with radiation, chemotherapy or combined chemoradiation. Tumour response was measured by growth delay. Hh transcript levels (qRT-PCR) were compared among frozen tumours from treated and control mice. 5E1, a monoclonal SHH antibody, or LDE225, a clinical SMO inhibitor (Novartis®) inhibited Hh signaling. RESULTS:Precision irradiation significantly delayed xenograft tumour growth in all 7 PDX models. Combined chemoradiation further delayed growth relative to either modality alone in three of six PDX models. Following irradiation, two of three PDX models demonstrated sustained up-regulation of Hh transcripts. Combined LDE225 and radiation, and 5E1 alone delayed growth relative to either treatment alone in a Hh-responsive PDX model, but not in a non-responsive model. CONCLUSION:Hh signaling mediates the radiation response in some EAC PDX models, and inhibition of this pathway may augment the efficacy of radiation in tumours that are Hh dependent.