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Replication-associated formation and repair of human topoisomerase IIIα cleavage complexes

Liton Kumar Saha, Sourav Saha, Xi Yang, Shar-yin N. Huang, Yilun Sun, Ukhyun Jo, Yves Pommier

2023Nature Communications23 citationsDOIOpen Access PDF

Abstract

Topoisomerase IIIα (TOP3A) belongs to the conserved Type IA family of DNA topoisomerases. Here we report that human TOP3A is associated with DNA replication forks and that a "self-trapping" TOP3A mutant (TOP3A-R364W) generates cellular TOP3A DNA cleavage complexes (TOP3Accs). We show that trapped TOP3Accs that interfere with replication, induce DNA damage and genome instability. To elucidate how TOP3Accs are repaired, we explored the role of Spartan (SPRTN), the metalloprotease associated with DNA replication, which digests proteins forming DNA-protein crosslinks (DPCs). We find that SPRTN-deficient cells show elevated TOP3Accs, whereas overexpression of SPRTN lowers cellular TOP3Accs. SPRTN is deubiquitinated and epistatic with TDP2 in response to TOP3Accs. In addition, we found that MRE11 can excise TOP3Accs, and that cell cycle determines the preference for the SPRTN-TDP2 vs. the ATM-MRE11 pathways, in S vs. G2, respectively. Our study highlights the prevalence of TOP3Accs repair mechanisms to ensure normal DNA replication.

Topics & Concepts

TopoisomeraseDNA replicationEukaryotic DNA replicationReplication protein AGenome instabilityDNA damageDNABiologyDNA repairCell biologyControl of chromosome duplicationCleavage (geology)Replication timingCell cycleMolecular biologyGeneticsChemistryDNA-binding proteinCellGeneTranscription factorFracture (geology)PaleontologyCancer therapeutics and mechanismsDNA Repair MechanismsPolyomavirus and related diseases
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