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Interplay of SMARCAD1 and BRCA1 at Replication Forks to Maintain Genome Integrity

Interplay of SMARCAD1 and BRCA1 at Replication Forks to Maintain Genome Integrity

Authors :
Hannes Lans
Nitika Taneja
Yifan Zhu
Arnab Ray Chaudhuri
Martin E. van Royen
Calvin Shun Yu Lo
Eleni Maria Manolika
Jos Jonkers
Chirantani Mukherjee
Marvin van Toorn
Vincent Gaggioli
David C. Wheeler
Wei Zhao
Ihor Smal
João G. S. C. Souto Gonçalves
Jurgen A. Marteijn
Jeroen Demmers
Mariana Paes Dias
Marit van der Does
Pim J. French
Source :
SSRN Electronic Journal.
Publication Year :
2020
Publisher :
Elsevier BV, 2020.

Abstract

Chemotherapeutic regimens that poison DNA replication are used for the treatment of homologous recombination (HR)-deficient cancers. We have discovered a novel mechanism by which the SWI/SNF chromatin remodeler SMARCAD1 stabilizes replication forks that is essential for resistance towards replication poisons. We find that loss of SMARCAD1 results in toxic enrichment of 53BP1 at replication forks which mediates untimely dissociation of PCNA via the PCNA-unloader, ATAD5. Faster dissociation of PCNA causes frequent fork stalling, inefficient fork restart and accumulation of single-stranded DNA resulting in genome instability. Although, loss of 53BP1 in SMARCAD1 mutants restore PCNA levels, fork restart efficiency, genome stability and resistance to replication poisons, this requires BRCA1 mediated fork protection. Interestingly, fork protection challenged BRCA1-deficient naive-or PARPi-resistant tumors require SMARCAD1 mediated fork stabilization to maintain cellular proliferation. Our data reveal a critical interplay between SMARCAD1 mediated fork stabilization and BRCA1 mediated fork protection in maintenance of genome stability.

Details

ISSN :
15565068
Database :
OpenAIRE
Journal :
SSRN Electronic Journal
Accession number :
edsair.doi...........55bfdf4c07b132e6d25763e658577b50
Full Text :
https://doi.org/10.2139/ssrn.3581365