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Mechanism for G2 phase-specific nuclear export of the kinetochore protein CENP-F

  • Kyle M. Loftus
  • , Heying Cui
  • , Elias Coutavas
  • , David S. King
  • , Amanda Ceravolo
  • , Dylan Pereiras
  • , Sozanne R. Solmaz

Research output: Contribution to journalArticlepeer-review

18 Scopus citations

Abstract

Centromere protein F (CENP-F) is a component of the kinetochore and a regulator of cell cycle progression. CENP-F recruits the dynein transport machinery and orchestrates several cell cycle-specific transport events, including transport of the nucleus, mitochondria and chromosomes. A key regulatory step for several of these functions is likely the G2 phase-specific export of CENP-F from the nucleus to the cytosol, where the cytoplasmic dynein transport machinery resides; however, the molecular mechanism of this process is elusive. Here, we have identified 3 phosphorylation sites within the bipartite classical nuclear localization signal (cNLS) of CENP-F. These sites are specific for cyclin-dependent kinase 1 (Cdk1), which is active in G2 phase. Phosphomimetic mutations of these residues strongly diminish the interaction of the CENP-F cNLS with its nuclear transport receptor karyopherin α. These mutations also diminish nuclear localization of the CENP-F cNLS in cells. Notably, the cNLS is phosphorylated in the −1 position, which is important to orient the adjacent major motif for binding into its pocket on karyopherin α. We propose that localization of CENP-F is regulated by a cNLS, and a nuclear export pathway, resulting in nuclear localization during most of interphase. In G2 phase, the cNLS is weakened by phosphorylation through Cdk1, likely resulting in nuclear export of CENP-F via the still active nuclear export pathway. Once CENP-F resides in the cytosol, it can engage in pathways that are important for cell cycle progression, kinetochore assembly and the faithful segregation of chromosomes into daughter cells.

Original languageEnglish
Pages (from-to)1414-1429
Number of pages16
JournalCell Cycle
Volume16
Issue number15
DOIs
StatePublished - Aug 3 2017

Keywords

  • centromere protein F
  • cyclin-dependent kinase 1
  • dynein
  • kinetochore
  • nuclear transport

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