A R-loop sensing pathway mediates the relocation of transcribed genes to nuclear pore complexes

Author:

Penzo AriannaORCID,Dubarry MarionORCID,Brocas Clémentine,Zheng MyriamORCID,Mangione Raphaël M.ORCID,Rougemaille MathieuORCID,Goncalves Coralie,Lautier Ophélie,Libri Domenico,Simon Marie-NoëlleORCID,Géli VincentORCID,Dubrana KarineORCID,Palancade BenoitORCID

Abstract

AbstractNuclear pore complexes (NPCs) have increasingly recognized interactions with the genome, as exemplified in yeast, where they bind transcribed or damaged chromatin. By combining genome-wide approaches with live imaging of model loci, we uncover a correlation between NPC association and the accumulation of R-loops, which are genotoxic structures formed through hybridization of nascent RNAs with their DNA templates. Manipulating hybrid formation demonstrates that R-loop accumulation per se, rather than transcription or R-loop-dependent damages, is the primary trigger for relocation to NPCs. Mechanistically, R-loop-dependent repositioning involves their recognition by the ssDNA-binding protein RPA, and SUMO-dependent interactions with NPC-associated factors. Preventing R-loop-dependent relocation leads to lethality in hybrid-accumulating conditions, while NPC tethering of a model hybrid-prone locus attenuates R-loop-dependent genetic instability. Remarkably, this relocation pathway involves molecular factors similar to those required for the association of stalled replication forks with NPCs, supporting the existence of convergent mechanisms for sensing transcriptional and genotoxic stresses.

Funder

Agence Nationale de la Recherche

Fondation ARC pour la Recherche sur le Cancer

Ligue Contre le Cancer

Fondation pour la Recherche Médicale

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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