G.O. Hellawell
Churchill Hospital
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Publication
Featured researches published by G.O. Hellawell.
Cancer Gene Therapy | 2005
Mark A. Rochester; Johann Riedemann; G.O. Hellawell; Simon Brewster; Valentine M. Macaulay
The type 1 insulin-like growth factor receptor (IGF1R) is overexpressed in prostate cancer, and mediates proliferation, motility, and survival. Many prostate cancers harbor inactivating PTEN mutations, enhancing Akt phosphorylation. This activates the principal antiapoptotic pathway downstream of the IGF1R, calling into question the value of IGF1R targeting in this tumor. The aim of the current study was to assess the effect of IGF1R gene silencing in prostate cancer cells that lack functional PTEN protein. In human DU145, LNCaP and PC3 prostate cancer cells, transfection with IGF1R small interfering RNA induced significant enhancement of apoptosis and inhibition of survival, not only in PTEN wild-type DU145 but also in PTEN mutant LNCaP and PC3. This was attributed to attenuation of IGF signaling via Akt, ERKs and p38. In both DU145 and PC3, IGF1R knockdown led to enhancement of sensitivity to mitoxantrone, etoposide, nitrogen mustard and ionizing radiation. There was no sensitization to paclitaxel or 5-fluorouracil, which do not damage DNA, suggesting that chemosensitization results from impairment of the DNA damage response, in addition to removal of apoptosis protection. These results support the concept of IGF1R targeting in prostate cancer, and indicate that PTEN loss does not render tumor cells refractory to this strategy.
BJUI | 2000
G.O. Hellawell; K.J. Turner; K.J. Le Monnier; Simon Brewster
Objective To determine the use of the Internet by urological patients for obtaining information about their disease, and to conduct an evaluation of urological websites to determine the quality of information available.
BJUI | 2003
G.O. Hellawell; D.J.P. Ferguson; Simon Brewster; Valentine M. Macaulay
To assess the effect of the downregulation of type 1 insulin‐like growth factor receptor (IGF1R) on the chemosensitivity of prostate cancer cells. IGF1R is overexpressed by prostate cancer compared with benign prostatic epithelium and IGF1R expression commonly persists in androgen‐independent metastatic disease at levels comparable to those in the primary.
Cancer Research | 2002
G.O. Hellawell; Gareth D. H. Turner; David R. Davies; Richard Poulsom; Simon Brewster; Valentine M. Macaulay
BJUI | 2002
G.O. Hellawell; Simon Brewster
European Urology Supplements | 2003
Mark A. Rochester; Nilay Patel; G.O. Hellawell; Simon Brewster; Valentine M. Macaulay
The Journal of Urology | 2004
Mark A. Rochester; Nilay Patel; G.O. Hellawell; Simon Brewster; Valentine M. Macaulay
European Urology Supplements | 2004
Mark A. Rochester; Nilay Patel; G.O. Hellawell; Simon Brewster; Valentine M. Macaulay
European Urology Supplements | 2003
G.O. Hellawell; Simon Brewster; Valentine M. Macaulay
European Urology Supplements | 2003
Mark A. Rochester; G.O. Hellawell; Simon Brewster; Valentine M. Macaulay