Plk1 overexpression induces chromosomal instability and suppresses tumor development.
Guillermo de CárcerSharavan Vishaan VenkateswaranLorena SalgueiroAicha El BakkaliKalman SomogyiKonstantina RowaldPablo MontañésManuel SanclementeBeatriz EscobarAlba de MartinoNicholas McGranahanMarcos MalumbresRocío SotilloPublished in: Nature communications (2018)
Polo-like kinase 1 (Plk1) is overexpressed in a wide spectrum of human tumors, being frequently considered as an oncogene and an attractive cancer target. However, its contribution to tumor development is unclear. Using a new inducible knock-in mouse model we report here that Plk1 overexpression results in abnormal chromosome segregation and cytokinesis, generating polyploid cells with reduced proliferative potential. Mechanistically, these cytokinesis defects correlate with defective loading of Cep55 and ESCRT complexes to the abscission bridge, in a Plk1 kinase-dependent manner. In vivo, Plk1 overexpression prevents the development of Kras-induced and Her2-induced mammary gland tumors, in the presence of increased rates of chromosome instability. In patients, Plk1 overexpression correlates with improved survival in specific breast cancer subtypes. Therefore, despite the therapeutic benefits of inhibiting Plk1 due to its essential role in tumor cell cycles, Plk1 overexpression has tumor-suppressive properties by perturbing mitotic progression and cytokinesis.
Keyphrases
- cell proliferation
- mouse model
- transcription factor
- high glucose
- endothelial cells
- end stage renal disease
- signaling pathway
- diabetic rats
- copy number
- induced apoptosis
- ejection fraction
- newly diagnosed
- gene expression
- squamous cell carcinoma
- oxidative stress
- cell therapy
- peritoneal dialysis
- mesenchymal stem cells
- papillary thyroid
- cell death
- cell cycle
- dna methylation
- patient reported outcomes
- bone marrow
- stress induced
- lymph node metastasis
- endoplasmic reticulum stress
- free survival