PLoS Genetics (Aug 2014)

Genetic deletion of SEPT7 reveals a cell type-specific role of septins in microtubule destabilization for the completion of cytokinesis.

  • Manoj B Menon,
  • Akihiro Sawada,
  • Anuhar Chaturvedi,
  • Pooja Mishra,
  • Karin Schuster-Gossler,
  • Melanie Galla,
  • Axel Schambach,
  • Achim Gossler,
  • Reinhold Förster,
  • Michael Heuser,
  • Alexey Kotlyarov,
  • Makoto Kinoshita,
  • Matthias Gaestel

DOI
https://doi.org/10.1371/journal.pgen.1004558
Journal volume & issue
Vol. 10, no. 8
p. e1004558

Abstract

Read online

Cytokinesis terminates mitosis, resulting in separation of the two sister cells. Septins, a conserved family of GTP-binding cytoskeletal proteins, are an absolute requirement for cytokinesis in budding yeast. We demonstrate that septin-dependence of mammalian cytokinesis differs greatly between cell types: genetic loss of the pivotal septin subunit SEPT7 in vivo reveals that septins are indispensable for cytokinesis in fibroblasts, but expendable in cells of the hematopoietic system. SEPT7-deficient mouse embryos fail to gastrulate, and septin-deficient fibroblasts exhibit pleiotropic defects in the major cytokinetic machinery, including hyperacetylation/stabilization of microtubules and stalled midbody abscission, leading to constitutive multinucleation. We identified the microtubule depolymerizing protein stathmin as a key molecule aiding in septin-independent cytokinesis, demonstrated that stathmin supplementation is sufficient to override cytokinesis failure in SEPT7-null fibroblasts, and that knockdown of stathmin makes proliferation of a hematopoietic cell line sensitive to the septin inhibitor forchlorfenuron. Identification of septin-independent cytokinesis in the hematopoietic system could serve as a key to identify solid tumor-specific molecular targets for inhibition of cell proliferation.