Valproic acid enhances tubulin acetylation and apoptotic activity of paclitaxel on anaplastic thyroid cancer cell lines

doi:10.1677/ERC-07-0096

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Endocrine-Related Cancer 14 (3) 839 -845 DOI: 10.1677/ERC-07-0096
Copyright © 2007 by the Society for Endocrinology

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Valproic acid enhances tubulin acetylation and apoptotic activity of paclitaxel on anaplastic thyroid cancer cell lines

Maria G Catalano¹, Roberta Poli², Mariateresa Pugliese², Nicoletta Fortunati² and Giuseppe Boccuzzi¹^,2

¹ Department of Clinical Pathophysiology, University of Turin, Via Genova, 3, 10126 Turin, Italy
² Oncological Endocrinology, ASO San Giovanni Battista, C.so Bramante 88, 10126 Turin, Italy

(Correspondence should be addressed to G Boccuzzi; Email: giuseppe.boccuzzi{at}unito.it)

The introduction of paclitaxel into multimodal therapy for anaplasticthyroid carcinoma has failed to improve overall survival. Toxicityrules out the high doses required, especially in older patients.The search for strategies to enhance paclitaxel antineoplasticactivity and reduce its side effects is thus advisable. Thestudy aimed to determine whether the histone deacetylase (HDAC)inhibitor valproic acid (VPA) improves the anticancer actionof paclitaxel and elucidate the mechanisms underlying the effectsof combined treatment. We examined the effect of VPA on thesensitivity to paclitaxel of two anaplastic thyroid carcinomacell lines (CAL-62 and ARO), and the ability of the drug todetermine tubulin acetylation and enhance paclitaxel-inducedacetylation. The addition of as little as 0.7 mM VPA to paclitaxelenhances both cytostatic and cytotoxic effects of paclitaxelalone. Increased apoptosis explains the enhancement of the cytotoxiceffect. The mechanism underlying this effect is through inhibitionof HDAC6 activity, which leads to tubulin hyperacetylation.The results suggest a mechanistic link between HDAC6 inhibition,tubulin acetylation, and the VPA-induced enhancement of paclitaxeleffects, and provide the rationale for designing future combinationtherapies.

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