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EXO1 as a therapeutic target for Fanconi Anaemia, ZRSR2 and BRCA1-A complex deficient cancers

EXO1 performs multiple roles in DNA replication and DNA damage repair (DDR), but its role in DDR-deficient cancers remains unclear. Here, the authors find EXO1 loss as synthetic lethal with many DDR genes involved in various cancers, including genes from Fanconi Anaemia pathway, BRCA1-A complex, and spliceosome factor ZRSR2; such interactions represent potential clinical targets.

Marija Maric
Sandra Segura-Bayona
Simon J. Boulton
ResearchOpen Access26 Sept 2025
Nature Communications

Volume: 16, P: 1-18
Mechanism of 53BP1 activity regulation by RNA-binding TIRR and a designer protein

Structural and functional dissection of the TIRR–53BP1 complex shows that TIRR acts as a regulatory switch that blocks 53BP1 binding to chromatin to direct DNA repair, and it releases 53BP1 in response to DNA damage by binding RNA.

Maria Victoria Botuyan
Gaofeng Cui
Georges Mer
Research02 Jul 2018
Nature Structural & Molecular Biology

Volume: 25, P: 591-600
TIRR regulates 53BP1 by masking its histone methyl-lysine binding function

A new protein, Tudor interacting repair regulator (TIRR), affects DNA repair by masking the chromatin interaction domain of 53BP1, thereby preventing its recruitment to double-strand breaks.

Pascal Drané
Marie-Eve Brault
Dipanjan Chowdhury
Research27 Feb 2017
Nature

Volume: 543, P: 211-216

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