| Literature DB >> 21779455 |
Sheng Yao1, Alix Bee, Daniel Brewer, Andrew Dodson, Carol Beesley, Youqiang Ke, Laurence Ambroisine, Gabrielle Fisher, Heinrich Møller, Tim Dickinson, Patricia Gerard, Lu-Yu Lian, Janet Risk, Brian Lane, Paul Smith, Victor Reuter, Daniel Berney, Christine Gosden, Peter Scardino, Jack Cuzick, Mustafa B A Djamgoz, Colin Cooper, Christopher S Foster.
Abstract
We show protein kinase C-zeta (PKC-ζ) to be a novel predictive biomarker for survival from prostate cancer (P < 0.001). We also confirm that transcription of the PRKC-ζ gene is crucial to the malignant phenotype of human prostate cancer. Following siRNA silencing of PRKC-ζ in PC3-M prostate cancer cells, stable transfectant cell line si-PRKC-ζ-PC3-M(T1-6) is phenotypically nonmalignant in vitro and in vivo. Genome-wide expression analysis identified 373 genes to be differentially expressed in the knockdown cells and 4 key gene networks to be significantly perturbed during phenotype modulation. Functional interconnection between some of the modulated genes is revealed, although these may be within different regulatory pathways, emphasizing the complexity of their mutual interdependence. Genes with altered expression following PRKC-ζ knockdown include HSPB1, RAD51, and ID1 that we have previously described to be critical in prostatic malignancy. Because expression of PRKC-ζ is functionally involved in promoting the malignant phenotype, we propose PKC-ζ as a novel and biologically relevant target for therapeutic intervention in prostate cancer.Entities:
Keywords: PRKC-ζ; prostate cancer; siRNA
Year: 2010 PMID: 21779455 PMCID: PMC3092210 DOI: 10.1177/1947601910376079
Source DB: PubMed Journal: Genes Cancer ISSN: 1947-6019