HDAC6 deacetylation of tubulin modulates dynamics of cellular adhesions

doi:10.1242/jcs.03431

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JCS ePress online publication date 27 Mar 2007
doi: 10.1242/jcs.03431

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Research Article

HDAC6 deacetylation of tubulin modulates dynamics of cellular adhesions

Andy Dong-Anh Tran, Timothy P. Marmo, Ambar A. Salam, Sally Che, Erik Finkelstein, Rafi Kabarriti, Harry S. Xenias, Ralph Mazitschek, Charlotte Hubbert, Yoshiharu Kawaguchi, Michael P. Sheetz, Tso-Pang Yao, and J. Chloë Bulinski^*
^* Author for correspondence (e-mail: jcb4{at}columbia.edu)

Genetic or pharmacological alteration of the activity of thehistone deacetylase 6 (HDAC6) induces a parallel alterationin cell migration. Using tubacin to block deacetylation of ${alpha}$ -tubulin,and not other HDAC6 substrates, yielded a motility reductionequivalent to agents that block all NAD-independent HDACs. Accordingly,we investigated how the failure to deacetylate tubulin contributesto decreased motility in HDAC6-inhibited cells. Testing thehypothesis that motility is reduced because cellular adhesionis altered, we found that inhibiting HDAC6 activity towardstubulin rapidly increased total adhesion area. Next, we investigatedthe mechanism of the adhesion area increase. Formation of adhesionsproceeded normally and cell spreading was more rapid in theabsence of active HDAC6; however, photobleaching assays andadhesion breakdown showed that adhesion turnover was slower.To test the role of hyperacetylated tubulin in altering adhesionturnover, we measured microtubule dynamics in HDAC6-inhibitedcells because dynamic microtubules are required to target adhesionsfor turnover. HDAC6 inhibition yielded a decrease in microtubuledynamics that was sufficient to decrease focal adhesion turnover.Thus, our results suggest a scenario in which the decreaseddynamics of hyperacetylated microtubules in HDAC6-inhibitedcells compromises their capacity to mediate the focal adhesiondynamics required for rapid cell migration.

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