The FIGNL1-FIRRM complex is required to complete meiotic recombination in the mouse and prevents massive DNA damage-independent RAD51 and DMC1 loading

Zainu, Akbar; Dupaigne, Pauline; Bouchouika, Soumya; Cau, Julien; Clément, Julie A. J.; Auffret, Pauline; Ropars, Virginie; Charbonnier, Jean-Baptiste; de Massy, Bernard; Mercier, Raphael; Kumar, Rajeev; Baudat, Frédéric

doi:10.1101/2023.05.17.541096

Cited by 2 publications

(1 citation statement)

References 120 publications

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“…S3). As expected and consistent with previous studies (17,22,26,29), FIGNL1N can dismantle RAD51 from both ssDNA and dsDNA (Fig. 2…”

Section: Fignl1 Atpase Is Essential For Rad51 Filament Disassemblysupporting

confidence: 92%

Molecular basis of FIGNL1 in dissociating RAD51 from DNA and chromatin

Carver,

Yu,

Yates

et al. 2024

Preprint

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Maintaining genome integrity is an essential and challenging process. RAD51 recombinase, the central player of several crucial processes in repairing and protecting genome integrity, forms filaments on DNA. RAD51 filaments are tightly regulated. One of these regulators is FIGNL1, that prevents persistent RAD51 foci post-damage and genotoxic chromatin association in cells. The cryogenic electron microscopy structure of FIGNL1 in complex with RAD51 reveals that the FIGNL1 forms a non-planar hexamer and RAD51 N-terminus is enclosed in the FIGNL1 hexamer pore. Mutations in pore loop or catalytic residues of FIGNL1 render it defective in filament disassembly and are lethal in mouse embryonic stem cells. Our study reveals a unique mechanism for removing RAD51 from DNA and provides the molecular basis for FIGNL1 in maintaining genome stability.

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“…S3). As expected and consistent with previous studies (17,22,26,29), FIGNL1N can dismantle RAD51 from both ssDNA and dsDNA (Fig. 2…”

Section: Fignl1 Atpase Is Essential For Rad51 Filament Disassemblysupporting

confidence: 92%

Molecular basis of FIGNL1 in dissociating RAD51 from DNA and chromatin

Carver,

Yu,

Yates

et al. 2024

Preprint

View full text Add to dashboard Cite

show abstract

FIGNL1 AAA+ ATPase remodels RAD51 and DMC1 filaments in pre-meiotic DNA replication and meiotic recombination

Ito,

Furukohri,

Matsuzaki

et al. 2023

Nat Commun

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The formation of RAD51/DMC1 filaments on single-stranded (ss)DNAs essential for homology search and strand exchange in DNA double-strand break (DSB) repair is tightly regulated. FIGNL1 AAA+++ ATPase controls RAD51-mediated recombination in human cells. However, its role in gametogenesis remains unsolved. Here, we characterized a germ line-specific conditional knockout (cKO) mouse of FIGNL1. Fignl1 cKO male mice showed defective chromosome synapsis and impaired meiotic DSB repair with the accumulation of RAD51/DMC1 on meiotic chromosomes, supporting a positive role of FIGNL1 in homologous recombination at a post-assembly stage of RAD51/DMC1 filaments. Fignl1 cKO spermatocytes also accumulate RAD51/DMC1 on chromosomes in pre-meiotic S-phase. These RAD51/DMC1 assemblies are independent of meiotic DSB formation. We also showed that purified FIGNL1 dismantles RAD51 filament on double-stranded (ds)DNA as well as ssDNA. These results suggest an additional role of FIGNL1 in limiting the non-productive assembly of RAD51/DMC1 on native dsDNAs during pre-meiotic S-phase and meiotic prophase I.

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The FIGNL1-FIRRM complex is required to complete meiotic recombination in the mouse and prevents massive DNA damage-independent RAD51 and DMC1 loading

Cited by 2 publications

References 120 publications

Molecular basis of FIGNL1 in dissociating RAD51 from DNA and chromatin

Molecular basis of FIGNL1 in dissociating RAD51 from DNA and chromatin

FIGNL1 AAA+ ATPase remodels RAD51 and DMC1 filaments in pre-meiotic DNA replication and meiotic recombination

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