4.7 Article

DYRK1B regulates Hedgehog-induced microtubule acetylation

Journal

CELLULAR AND MOLECULAR LIFE SCIENCES
Volume 76, Issue 1, Pages 193-207

Publisher

SPRINGER BASEL AG
DOI: 10.1007/s00018-018-2942-5

Keywords

Hedgehog; SHH; DYRK1B; HDAC6; GSK3; Microtubules; Acetylation; Organelle transport; Cell migration

Funding

  1. German Research Society [DFG-KFO325, DFG-LA2829/9-1]
  2. Behring-Rontgen Foundation
  3. University Hospital Giessen-Marburg (UKGM)

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The posttranslational modification (PTM) of tubulin subunits is important for the physiological functions of the microtubule (MT) cytoskeleton. Although major advances have been made in the identification of enzymes carrying out MT-PTMs, little knowledge is available on how intercellular signaling molecules and their associated pathways regulate MT-PTM-dependent processes inside signal-receiving cells. Here we show that Hedgehog (Hh) signaling, a paradigmatic intercellular signaling system, affects the MT acetylation state in mammalian cells. Mechanistically, Hh pathway activity increases the levels of the MT-associated DYRK1B kinase, resulting in the inhibition of GSK3 through phosphorylation of Serine 9 and the subsequent suppression of HDAC6 enzyme activity. Since HDAC6 represents a major tubulin deacetylase, its inhibition increases the levels of acetylated MTs. Through the activation of DYRK1B, Hh signaling facilitates MT-dependent processes such as intracellular mitochondrial transport, mesenchymal cell polarization or directed cell migration. Taken together, we provide evidence that intercellular communication through Hh signals can regulate the MT cytoskeleton and contribute to MT-dependent processes by affecting the level of tubulin acetylation.

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