Literature DB >> 31953325

The disordered N-terminus of HDAC6 is a microtubule-binding domain critical for efficient tubulin deacetylation.

Kseniya Ustinova1, Zora Novakova2, Makoto Saito3, Marat Meleshin4, Jana Mikesova2, Zsofia Kutil2, Petra Baranova2, Barbora Havlinova2, Mike Schutkowski4, Patrick Matthias3, Cyril Barinka5.   

Abstract

Histone deacetylase 6 (HDAC6) is a multidomain cytosolic enzyme having tubulin deacetylase activity that has been unequivocally assigned to the second of the tandem catalytic domains. However, virtually no information exists on the contribution of other HDAC6 domains on tubulin recognition. Here, using recombinant protein expression, site-directed mutagenesis, fluorimetric and biochemical assays, microscale thermophoresis, and total internal reflection fluorescence microscopy, we identified the N-terminal, disordered region of HDAC6 as a microtubule-binding domain and functionally characterized it to the single-molecule level. We show that the microtubule-binding motif spans two positively charged patches comprising residues Lys-32 to Lys-58. We found that HDAC6-microtubule interactions are entirely independent of the catalytic domains and are mediated by ionic interactions with the negatively charged microtubule surface. Importantly, a crosstalk between the microtubule-binding domain and the deacetylase domain was critical for recognition and efficient deacetylation of free tubulin dimers both in vitro and in vivo Overall, our results reveal that recognition of substrates by HDAC6 is more complex than previously appreciated and that domains outside the tandem catalytic core are essential for proficient substrate deacetylation.
© 2020 Ustinova et al.

Entities:  

Keywords:  cytoskeleton; histone deacetylase 6 (HDAC6); intrinsically disordered protein; microtubule-associated protein (MAP); post-translational modification; protein motif; protein-protein interaction; structure-function; substrate specificity; total internal reflection fluorescence (TIRF); tubulin

Mesh:

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Year:  2020        PMID: 31953325      PMCID: PMC7049964          DOI: 10.1074/jbc.RA119.011243

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


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