Litcius/Paper detail

BMI-1 regulates DNA end resection and homologous recombination repair

Amira Fitieh, Andrew J. Locke, Fatemeh Mashayekhi, Fajr Khaliqdina, Ajit Kumar Sharma, Ismail Hassan Ismail

2022Cell Reports31 citationsDOIOpen Access PDF

Abstract

BMI-1 is an essential regulator of transcriptional silencing during development. Recently, the role of BMI-1 in the DNA damage response has gained much attention, but the exact mechanism of how BMI-1 participates in the process is unclear. Here, we establish a role for BMI-1 in the repair of DNA double-strand breaks by homologous recombination (HR), where it promotes DNA end resection. Mechanistically, BMI-1 mediates DNA end resection by facilitating the recruitment of CtIP, thus allowing RPA and RAD51 accumulation at DNA damage sites. Interestingly, treatment with transcription inhibitors rescues the DNA end resection defects of BMI-1-depleted cells, suggesting BMI-1-dependent transcriptional silencing mediates DNA end resection. Moreover, we find that H2A ubiquitylation at K119 (H2AK119ub) promotes end resection. Taken together, our results identify BMI-1-mediated transcriptional silencing and promotion of H2AK119ub deposition as essential regulators of DNA end resection and thus the progression of HR.

Topics & Concepts

RAD51Homologous recombinationDNA damageGene silencingNon-homologous end joiningDNA repairBiologyDNAResectionCell biologyGeneticsGeneMedicineSurgeryDNA Repair MechanismsPARP inhibition in cancer therapyEpigenetics and DNA Methylation