Abstract:Kinesin‐5 proteins are essential for formation of a bipolar mitotic spindle in eukaryotic cells. Notably, the human Kinesin‐5 motor, HsEg5, is a target for an expanding group of small‐molecule inhibitors that hold promise both as tools to probe mechanochemical transduction and as anti‐cancer agents. Although most such compounds are selective for HsEg5, some exhibit activity against at least one kinesin from outside the Kinesin‐5 subfamily. Here we show NSC 622124, despite identification in an inhibitor screen … Show more
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