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Simple solutions to complex problems: from cell cycle regulation to anti-cancer treatments

Simple solutions to complex problems: from cell cycle regulation to anti-cancer treatments

University of Dundee

My lab investigates how signalling networks regulate cell cycle transitions and how these can be targeted to treat cancer. Our work spans fundamental to translational research and I will cover both of these areas in the two parts of my seminar.

Part I: The origins of complexity in protein phosphorylation networks

I will start by discussing a fundamental property that is common to all phosphorylation sites, but for which almost nothing is currently known: the rate that these sites can 鈥渇lash鈥 on and off over time. I will briefly highlight how we plan to tackle this problem over the coming years, before presenting our recent unpublished data on a bifunctional kinase-phosphatase module that induces such dynamic phosphorylation-dephosphorylation cycles to coordinate two key mitotic processes.

Part II: Cell cycle inhibitors can switch an oncogene into a tumour suppressor

I will then switch focus to highlight how understanding simple concepts in cell cycle and growth control can help to answer an age-old question in cancer research: how can cell cycle inhibitors be used to selectively target cancer cells? The work I will present, which is also largely unpublished, will explain how CDK4/6 inhibitors can induce selective toxicity in tumour cells that are primed for oncogenic cell growth.

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