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Mechanisms of HsSAS-6 assembly promoting centriole formation in human cells

  • Debora Keller
  • , Meritxell Orpinell
  • , Nicolas Olivier
  • , Malte Wachsmuth
  • , Robert Mahen
  • , Romain Wyss
  • , Virginie Hachet
  • , Jan Ellenberg
  • , Suliana Manley
  • , Pierre Gönczy
  • School of Life Sciences
  • Imperial College London
  • Laboratory for Experimental Biophysics
  • King's College London
  • European Molecular Biology Laboratory Heidelberg
  • ENAC-IIC-GEL

Résultats de recherche: Contribution à un journalArticleRevue par des pairs

Résumé

SAS-6 proteins are thought to impart the ninefold symmetry of centrioles, but the mechanisms by which their assembly occurs within cells remain elusive. In this paper, we provide evidence that the N-terminal, coiled-coil, and C-terminal domains of HsSAS-6 are each required for procentriole formation in human cells. Moreover, the coiled coil is necessary and sufficient to mediate HsSAS-6 centrosomal targeting. High-resolution imaging reveals that GFP-tagged HsSAS-6 variants localize in a torus around the base of the parental centriole before S phase, perhaps indicative of an initial loading platform. Moreover, fluorescence recovery after photobleaching analysis demonstrates that HsSAS-6 is immobilized progressively at centrosomes during cell cycle progression. Using fluorescence correlation spectroscopy and threedimensional stochastic optical reconstruction microscopy, we uncover that HsSAS-6 is present in the cytoplasm primarily as a homodimer and that its oligomerization into a ninefold symmetrical ring occurs at centrioles. Together, our findings lead us to propose a mechanism whereby HsSAS-6 homodimers are targeted to centrosomes where the local environment and high concentration of HsSAS-6 promote oligomerization, thus initiating procentriole formation.

langue originaleAnglais
Pages (de - à)697-712
Nombre de pages16
journalJournal of Cell Biology
Volume204
Numéro de publication5
Les DOIs
étatPublié - 1 janv. 2014
Modification externeOui

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