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IGF-1R associates with adverse outcomes after radical radiotherapy for prostate cancer

Authors :
Clare Verrill
S. Larrè
Richard J. Bryant
Tamara Aleksic
Laurent Brureau
Syed Haider
Valentine M. Macaulay
Cheng Han
Andrew Ross Worrall
Ahmad Sabbagh
David Cole
Fahad Fazal
Francesca M. Buffa
Geoff S. Higgins
Source :
British Journal of Cancer
Publication Year :
2017

Abstract

Background: Activated type 1 insulin-like growth factor receptors (IGF-1Rs) undergo internalisation and nuclear translocation, promoting cell survival. We previously reported that IGF-1R inhibition delays DNA damage repair, sensitising prostate cancer cells to ionising radiation. Here we tested the clinical relevance of these findings. Methods: We assessed associations between IGF-1R and clinical outcomes by immunohistochemistry in diagnostic biopsies of 136 men treated with 55–70 Gy external beam radiotherapy for prostate cancer, comparing results with publicly available transcriptional data in surgically treated patients. Results: Following radiotherapy, overall recurrence-free survival was shorter in patients whose tumours contained high total, cytoplasmic and internalised (nuclear/cytoplasmic) IGF-1R. High total IGF-1R associated with high primary Gleason grade and risk of metastasis, and cytoplasmic and internalised IGF-1R with biochemical recurrence, which includes patients experiencing local recurrence within the radiation field indicating radioresistance. In multivariate analysis, cytoplasmic, internalised and total IGF-1R were independently associated with risk of overall recurrence, and cytoplasmic IGF-1R was an independent predictor of biochemical recurrence post radiotherapy. Insulin-like growth factor receptors expression did not associate with biochemical recurrence after radical prostatectomy. Conclusions: These data reveal increased risk of post-radiotherapy recurrence in men whose prostate cancers contain high levels of total or cytoplasmic IGF-1R.

Details

ISSN :
15321827
Volume :
117
Issue :
11
Database :
OpenAIRE
Journal :
British journal of cancer
Accession number :
edsair.doi.dedup.....c7778fdb126537742f17354fbd102e3e