Cancers (Jan 2020)

Dephosphorylation of YB-1 is Required for Nuclear Localisation During G<sub>2</sub> Phase of the Cell Cycle

  • Sunali Mehta,
  • Cushla McKinney,
  • Michael Algie,
  • Chandra S. Verma,
  • Srinivasaraghavan Kannan,
  • Rhodri Harfoot,
  • Tara K. Bartolec,
  • Puja Bhatia,
  • Alistair J. Fisher,
  • Maree L. Gould,
  • Kim Parker,
  • Anthony J. Cesare,
  • Heather E. Cunliffe,
  • Scott B. Cohen,
  • Torsten Kleffmann,
  • Antony W. Braithwaite,
  • Adele G. Woolley

DOI
https://doi.org/10.3390/cancers12020315
Journal volume & issue
Vol. 12, no. 2
p. 315

Abstract

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Elevated levels of nuclear Y-box binding protein 1 (YB-1) are linked to poor prognosis in cancer. It has been proposed that entry into the nucleus requires specific proteasomal cleavage. However, evidence for cleavage is contradictory and high YB-1 levels are prognostic regardless of cellular location. Here, using confocal microscopy and mass spectrometry, we find no evidence of specific proteolytic cleavage. Doxorubicin treatment, and the resultant G2 arrest, leads to a significant increase in the number of cells where YB-1 is not found in the cytoplasm, suggesting that its cellular localisation is variable during the cell cycle. Live cell imaging reveals that the location of YB-1 is linked to progression through the cell cycle. Primarily perinuclear during G1 and S phases, YB-1 enters the nucleus as cells transition through late G2/M and exits at the completion of mitosis. Atomistic modelling and molecular dynamics simulations show that dephosphorylation of YB-1 at serine residues 102, 165 and 176 increases the accessibility of the nuclear localisation signal (NLS). We propose that this conformational change facilitates nuclear entry during late G2/M. Thus, the phosphorylation status of YB-1 determines its cellular location.

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