Critical Role for Cold Shock Protein YB-1 in Cytokinesis.
Sunali Y MehtaMichael AlgieTariq Al-JabryCushla McKinneySrinivasaraghavan KannanChandra Shekhar VermaWeini MaJessie ZhangTara K BartolecV Pragathi MasamsettiKim ParkerLuke HendersonMaree L GouldPuja BhatiaRhodri HarfootMegan ChircopTorsten KleffmannScott B CohenAdele G WoolleyAnthony J CesareAntony BraithwaitePublished in: Cancers (2020)
High levels of the cold shock protein Y-box-binding protein-1, YB-1, are tightly correlated with increased cell proliferation and progression. However, the precise mechanism by which YB-1 regulates proliferation is unknown. Here, we found that YB-1 depletion in several cancer cell lines and in immortalized fibroblasts resulted in cytokinesis failure and consequent multinucleation. Rescue experiments indicated that YB-1 was required for completion of cytokinesis. Using confocal imaging we found that YB-1 was essential for orchestrating the spatio-temporal distribution of the microtubules, β-actin and the chromosome passenger complex (CPC) to define the cleavage plane. We show that phosphorylation at six serine residues was essential for cytokinesis, of which novel sites were identified using mass spectrometry. Using atomistic modelling we show how phosphorylation at multiple sites alters YB-1 conformation, allowing it to interact with protein partners. Our results establish phosphorylated YB-1 as a critical regulator of cytokinesis, defining precisely how YB-1 regulates cell division.
Keyphrases
- energy transfer
- binding protein
- cell proliferation
- mass spectrometry
- high resolution
- transcription factor
- signaling pathway
- protein kinase
- molecular dynamics simulations
- stem cells
- protein protein
- single cell
- amino acid
- small molecule
- hepatitis c virus
- young adults
- liquid chromatography
- cell therapy
- genome wide
- photodynamic therapy
- papillary thyroid
- human immunodeficiency virus
- ms ms
- bone marrow
- fluorescence imaging
- pi k akt