CDK12 controls transcription at damaged genes and prevents MYC-induced transcription-replication conflicts.
Laura CurtiSara RohbanNicola BianchiOttavio CrociAdrian AndronacheSara BarozziMichela MattioliFernanda RicciElena PastoriSilvia SbernaSimone BellottiAnna AccialiniRoberto BallarinoNicola CrosettoMark WadeDario ParazzoliStefano CampanerPublished in: Nature communications (2024)
The identification of genes involved in replicative stress is key to understanding cancer evolution and to identify therapeutic targets. Here, we show that CDK12 prevents transcription-replication conflicts (TRCs) and the activation of cytotoxic replicative stress upon deregulation of the MYC oncogene. CDK12 was recruited at damaged genes by PARP-dependent DDR-signaling and elongation-competent RNAPII, to repress transcription. Either loss or chemical inhibition of CDK12 led to DDR-resistant transcription of damaged genes. Loss of CDK12 exacerbated TRCs in MYC-overexpressing cells and led to the accumulation of double-strand DNA breaks, occurring between co-directional early-replicating regions and transcribed genes. Overall, our data demonstrate that CDK12 protects genome integrity by repressing transcription of damaged genes, which is required for proper resolution of DSBs at oncogene-induced TRCs. This provides a rationale that explains both how CDK12 deficiency can promote tandem duplications of early-replicated regions during tumor evolution, and how CDK12 targeting can exacerbate replicative-stress in tumors.
Keyphrases
- cell cycle
- transcription factor
- genome wide
- bioinformatics analysis
- genome wide identification
- cell proliferation
- high glucose
- dna damage
- dna methylation
- single molecule
- genome wide analysis
- electronic health record
- clinical trial
- deep learning
- squamous cell carcinoma
- big data
- drug induced
- papillary thyroid
- machine learning
- cell death
- cell free
- data analysis
- replacement therapy