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Showing papers by "John I. Risinger published in 2009"

Journal ArticleDOI
Melanoma antigen-11 inhibits the hypoxia-inducible factor prolyl hydroxylase 2 and activates hypoxic response.

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Olga Aprelikova1, Olga Aprelikova2, Silvia Pandolfi2, Sean Tackett2, Mark Ferreira2, Konstantin Salnikow2, Yvona Ward2, John I. Risinger2, J. Carl Barrett2, John E. Niederhuber2 
Novartis1, National Institutes of Health2
15 Jan 2009-Cancer Research
TL;DR: Inhibition of PHD by MAGE-11, and following activation of HIFs, is a novel tumor-associated HIF regulatory mechanism that may provide valuable tools for therapeutic intervention because of the restricted expression of the MAGE gene family in cancers, but not in normal tissues.
Abstract: Activation of hypoxia-inducible factors (HIF), responsible for tumor angiogenesis and glycolytic switch, is regulated by reduced oxygen availability. Normally, HIF-alpha proteins are maintained at low levels, controlled by site-specific hydroxylation carried out by HIF prolyl hydroxylases (PHD) and subsequent proteasomal degradation via the von Hippel-Lindau ubiquitin ligase. Using a yeast two-hybrid screen, we identified an interaction between melanoma antigen-11 (MAGE-11) cancer-testis antigen and the major HIF-alpha hydroxylating enzyme PHD2. The interaction was confirmed by a pull-down assay, coimmunoprecipitation, and colocalization in both normoxic and hypoxic conditions. Furthermore, MAGE-9, the closest homologue of MAGE-11, was also found to interact with PHD2. MAGE-11 inhibited PHD activity without affecting protein levels. This inhibition was accompanied by stabilization of ectopic or endogenous HIF-1alpha protein. Knockdown of MAGE-11 by small interfering RNA results in decreased hypoxic induction of HIF-1alpha and its target genes. Inhibition of PHD by MAGE-11, and following activation of HIFs, is a novel tumor-associated HIF regulatory mechanism. This finding provides new insights into the significance of MAGE expression in tumors and may provide valuable tools for therapeutic intervention because of the restricted expression of the MAGE gene family in cancers, but not in normal tissues.

53 citations

Journal ArticleDOI
Serum S100A6 Concentration Predicts Peritoneal Tumor Burden in Mice with Epithelial Ovarian Cancer and Is Associated with Advanced Stage in Patients

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Bih Rong Wei1, Shelley B. Hoover1, Mark M. Ross2, Weidong Zhou2, Francesco Meani3, Jeniffer B. Edwards1, Elizabeth Spehalski, John I. Risinger, W. Gregory Alvord1, Octavio A. Quiñones1, Claudio Belluco4, Luca Martella, Elio Campagnutta, Antonella Ravaggi3, Rei Ming Dai1, Paul K. Goldsmith1, Kevin D. Woolard1, Sergio Pecorelli3, Lance A. Liotta2, Emanuel F. Petricoin2, R. Mark Simpson1 
National Institutes of Health1, George Mason University2, University of Brescia3, Istituto Superiore di Sanità4
30 Oct 2009-PLOS ONE
TL;DR: S100A6 is found in serum in concentrations that correlate with experimental tumor burden and with clinical disease stage, and may prove useful in detecting and/or monitoring ovarian cancer, when used in concert with other biomarkers.
Abstract: Background Ovarian cancer is the 5th leading cause of cancer related deaths in women. Five-year survival rates for early stage disease are greater than 94%, however most women are diagnosed in advanced stage with 5 year survival less than 28%. Improved means for early detection and reliable patient monitoring are needed to increase survival.

40 citations