U. Foerstermann scite author profile

U. Foerstermann

3Publications

74Citation Statements Received

148Citation Statements Given

How they've been cited

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141

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Johannes Gutenberg University Mainz

Publications

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Protectors or Traitors: The Roles of PON2 and PON3 in Atherosclerosis and Cancer

Witte

Foerstermann²,

Devarajan³

et al. 2012

Journal of Lipids

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Cancer and atherosclerosis are major causes of death in western societies. Deregulated cell death is common to both diseases, with significant contribution of inflammatory processes and oxidative stress. These two form a vicious cycle and regulate cell death pathways in either direction. This raises interest in antioxidative systems. The human enzymes paraoxonase-2 (PON2) and PON3 are intracellular enzymes with established antioxidative effects and protective functions against atherosclerosis. Underlying molecular mechanisms, however, remained elusive until recently. Novel findings revealed that both enzymes locate to mitochondrial membranes where they interact with coenzyme Q10 and diminish oxidative stress. As a result, ROS-triggered mitochondrial apoptosis and cell death are reduced. From a cardiovascular standpoint, this is beneficial given that enhanced loss of vascular cells and macrophage death forms the basis for atherosclerotic plaque development. However, the same function has now been shown to raise chemotherapeutic resistance in several cancer cells. Intriguingly, PON2 as well as PON3 are frequently found upregulated in tumor samples. Here we review studies reporting PON2/PON3 deregulations in cancer, summarize most recent findings on their anti-oxidative and antiapoptotic mechanisms, and discuss how this could be used in putative future therapies to target atherosclerosis and cancer.

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Po9-246 Human Paraoxonase 2: An Endogenous Enzyme as Defense System Against Vascular Oxidative Stress and Endoplasmic Reticulum Stress-Induced Apoptosis

Horke¹,

Witte²,

Wilgenbus³

et al. 2007

Atherosclerosis Supplements

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ChemInform Abstract: Inhibitors of Inducible NO Synthase Expression: Total Synthesis of (S)‐Curvularin (Ia) and Its Ring Homologues.

et al. 2008

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Other bioactive products U 1300Inhibitors of Inducible NO Synthase Expression: Total Synthesis of (S)-Curvularin (Ia) and Its Ring Homologues. -The derivatives (II) show improved downregulation of iNOS expression and almost no negative effects on eNOS expression as is desirable for antiinflammatory drugs. -(ELZNER, S.; SCHMIDT, D.; SCHOLLMEYER, D.; ERKEL, G.; ANKE, T.; KLEINERT, H.; FOERSTERMANN, U.; KUNZ*, H.; ChemMedChem 3 (2008) 6, 924-939; Inst. Org. Chem., Johannes-Gutenberg-Univ., D-55128 Mainz, Germany; Eng.) -Bartels 42-210

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U. Foerstermann

Protectors or Traitors: The Roles of PON2 and PON3 in Atherosclerosis and Cancer

Po9-246 Human Paraoxonase 2: An Endogenous Enzyme as Defense System Against Vascular Oxidative Stress and Endoplasmic Reticulum Stress-Induced Apoptosis

ChemInform Abstract: Inhibitors of Inducible NO Synthase Expression: Total Synthesis of (S)‐Curvularin (Ia) and Its Ring Homologues.

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