Extra centrosomes delay DNA damage-driven tumorigenesis.
Vincent Z BraunGerlinde KarbonFabian SchulerMarina A SchapflJohannes G WeissPaul Y PetermannDiana Carolina Johanna SpieringsAndréa E TijhuisFloris FoijerVerena LabiAndreas VillungerPublished in: Science advances (2024)
Deregulated centrosome numbers are frequently found in human cancer and can promote malignancies in model organisms. Current research aims to clarify if extra centrosomes are cause or consequence of malignant transformation, and if their biogenesis can be targeted for therapy. Here, we show that oncogene-driven blood cancer is inert to genetic manipulation of centrosome numbers, whereas the formation of DNA damage-induced malignancies is delayed. We provide first evidence that this unexpected phenomenon is connected to extra centrosomes eliciting a pro-death signal engaging the apoptotic machinery. Apoptosis induction requires the PIDDosome multi-protein complex, as it can be abrogated by loss of any of its three components, Caspase-2 , Raidd/Cradd , or Pidd1 . BCL2 overexpression equally blocks cell death, documenting for the first time induction of mitochondrial apoptosis downstream of extra centrosomes. Our findings demonstrate context-dependent effects of centrosome amplification during transformation and ask to adjust current belief that extra centrosomes are intrinsically pro-tumorigenic.
Keyphrases
- cell death
- dna damage
- oxidative stress
- cell cycle arrest
- papillary thyroid
- diabetic rats
- anti inflammatory
- endothelial cells
- induced apoptosis
- dna methylation
- cell proliferation
- stem cells
- cancer therapy
- genome wide
- signaling pathway
- squamous cell carcinoma
- lymph node metastasis
- copy number
- childhood cancer
- pluripotent stem cells
- smoking cessation
- label free
- cell therapy