Long-molecule scars of backup DNA repair in BRCA1- and BRCA2-deficient cancers

Setton, J.; Hadi, Kevin; Choo, Zi-Ning; Kuchin, Katerina; Tian, Huasong; Paula, Arnaud Da Cruz; Rosiene, Joel; Selenica, Pier; Behr, Julie M.; Yao, Xiaotong; Deshpande, Aditya; Sigouros, Michael; Manohar, Jyothi; Nauseef, Jones T.; Mosquera, Juan Miguel; Elemento, Olivier; Weigelt, Britta; Riaz, Nadeem; Reis‐Filho, Jorge S.; Powell, Simon N.; Imieliński, Marcin

doi:10.1038/s41586-023-06461-2

Cited by 8 publications

(1 citation statement)

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“…This mechanism would be of special importance in the context of highly repetitive genome regions, where multi-invasions may lead to cycles of deletion or expansion of repeated sequences. It could also be responsible for some structural variants (characterized by large chromosomal aberrations) that arise during cancerogenesis in the BRCA-deficient context ( 88 ).…”

Section: Discussionmentioning

confidence: 99%

Human RAD52 stimulates the RAD51-mediated homology search

Muhammad,

Basto,

Peterlini

et al. 2023

Life Sci. Alliance

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Homologous recombination (HR) is a DNA repair mechanism of double-strand breaks and blocked replication forks, involving a process of homology search leading to the formation of synaptic intermediates that are regulated to ensure genome integrity. RAD51 recombinase plays a central role in this mechanism, supported by its RAD52 and BRCA2 partners. If the mediator function of BRCA2 to load RAD51 on RPA-ssDNA is well established, the role of RAD52 in HR is still far from understood. We used transmission electron microscopy combined with biochemistry to characterize the sequential participation of RPA, RAD52, and BRCA2 in the assembly of the RAD51 filament and its activity. Although our results confirm that RAD52 lacks a mediator activity, RAD52 can tightly bind to RPA-coated ssDNA, inhibit the mediator activity of BRCA2, and form shorter RAD51-RAD52 mixed filaments that are more efficient in the formation of synaptic complexes and D-loops, resulting in more frequent multi-invasions as well. We confirm the in situ interaction between RAD51 and RAD52 after double-strand break induction in vivo. This study provides new molecular insights into the formation and regulation of presynaptic and synaptic intermediates by BRCA2 and RAD52 during human HR.

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Section: Discussionmentioning

confidence: 99%