4.8 Article

A Family of Protein-Deglutamylating Enzymes Associated with Neurodegeneration

Journal

CELL
Volume 143, Issue 4, Pages 564-578

Publisher

CELL PRESS
DOI: 10.1016/j.cell.2010.10.014

Keywords

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Funding

  1. CNRS
  2. Universities Montpellier
  3. Institut Curie
  4. Association pour la Recherche sur le Cancer (ARC) [3140, 4892, 7927]
  5. French National Research Agency (ANR) [05-JCJC-0035, 08-JCJC-0007]
  6. Fondation pour la Recherche Medicale (FRM) [DEQ20081213977]
  7. HFSP [RGP 23/2008]
  8. EMBO [R07Job, ASTF 157-2007, ALTF 546-2006]
  9. Alzheimer Forschung Initiative [06825]
  10. La Ligue contre le Cancer

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Polyglutamylation is a posttranslational modification that generates glutamate side chains on tubulins and other proteins. Although this modification has been shown to be reversible, little is known about the enzymes catalyzing deglutamylation. Here we describe the enzymatic mechanism of protein deglutamylation by members of the cytosolic carboxypeptidase (CCP) family. Three enzymes (CCP1, CCP4, and CCP6) catalyze the shortening of polyglutamate chains and a fourth (CCP5) specifically removes the branching point glutamates. In addition, CCP1, CCP4, and CCP6 also remove gene-encoded glutamates from the carboxyl termini of proteins. Accordingly, we show that these enzymes convert detyrosinated tubulin into Delta 2-tubulin and also modify other substrates, including myosin light chain kinase 1. We further analyze Purkinje cell degeneration (pcd) mice that lack functional CCP1 and show that microtubule hyperglutamylation is directly linked to neurodegeneration. Taken together, our results reveal that controlling the length of the polyglutamate side chains on tubulin is critical for neuronal survival.

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