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Inhibition of cell migration and cell division correlates with distinct effects of microtubule inhibiting drugs.

The Journal of biological chemistry (2010-08-11)
Hailing Yang, Anutosh Ganguly, Fernando Cabral
RESUMEN

Drugs that target microtubules are thought to inhibit cell division and cell migration by suppressing dynamic instability, a "search and capture" behavior that allows microtubules to probe their environment. Here, we report that subtoxic drug concentrations are sufficient to inhibit plus-end microtubule dynamic instability and cell migration without affecting cell division or microtubule assembly. The higher drug concentrations needed to inhibit cell division act through a novel mechanism that generates microtubule fragments by stimulating microtubule minus-end detachment from their organizing centers. The frequency of microtubule detachment in untreated cells increases at prophase suggesting that it is a regulated cellular process important for spindle assembly and function. We conclude that drugs produce differential dose-dependent effects at microtubule plus and minus-ends to inhibit different microtubule-mediated functions.

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Sigma-Aldrich
Demecolcine solution, 10 μg/mL in HBSS, ACF Qualified, BioXtra
Sigma-Aldrich
Demecolcine, ≥98% (HPLC)