Article ID Journal Published Year Pages File Type
2785951 International Journal of Developmental Neuroscience 2014 6 Pages PDF
Abstract

•The cell viability was found significantly decreased over time in the SCA3-Q84 cell line, whereas remained unchanged in the SCA3-Q28 cell line.•VPA significantly improved the SCA3-Q84 cell viability and suppressed expanded polyQ-induced cytotoxicity, but not the number of inclusions.•Expanded ataxin-3 suppressed the expression of acetylated histone H3 while VPA reversed the histone hypoacetylation.•VPA attenuates the expanded polyQ-induced down-regulation of CRE-dependent transcriptional activation.

Machado–Joseph disease (MJD) is caused by a (CAG)n trinucleotide repeat expansion that is translated into an abnormally long polyglutamine tract. This disease is considered the most common form of spinocerebellar ataxia (SCA). In the present study, we developed stable inducible cell lines (PC12Tet-On-Ataxin-3-Q28/84) expressing ataxin-3 with either normal or abnormal CAG repeats under doxycycline control. The expression of acetyl histone H3 and the induction of c-Fos in response to cAMP were strongly suppressed in cells expressing the protein with the expanded polyglutamine tract. Treatment with valproic acid, a histone deacetylase inhibitor (HDACi), attenuated mutant ataxin-3-induced cell toxicity and suppression of acetyl histone H3, phosphorylated cAMP-responsive element binding protein (p-CREB) as well as c-Fos expression. These results indicate that VPA can stimulate the up-regulation of gene transcription through hyperacetylation. Thus, VPA might have a therapeutic effect on MJD.

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