Defective Microhomology-Mediated End-joining in SMARCB1-Deficient Tumors.

Publication information:

Zhu, G. et al. Defective Microhomology-Mediated End-joining in SMARCB1-Deficient Tumors. bioRxiv : the preprint server for biology (2025) doi:10.1101/2025.11.20.689563.

Abstract

Rhabdoid tumors (RTs) are highly aggressive cancers driven by biallelic mutation of a core subunit of the BAF (SWI/SNF) complex. We found that SMARCB1-deficient tumors have a defect in the microhomology-mediated end-joining (MMEJ) pathway, and SMARCB1 is essential for maintaining the protein level of the core MMEJ protein Polymerase Q (POLQ). Mechanistically, SMARCB1 facilitates the nuclear export of the mRNA through its interaction with the nuclear pore complex. Interestingly, loss of MMEJ in RT cells leads to a compensatory activation of, and a hyper-dependence on, the Fanconi Anemia (FA)/BRCA pathway. Knockout or inhibition of this pathway selectively kills RT cells. Notably, RBM39 degraders, novel splicing modulators, effectively inhibit the FA/BRCA pathway and kill RT cells. SMARCB1 and other cBAF/pBAF components are important for maintenance of MMEJ activity and POLQ protein level, suggesting that BAF-deficient cancers more broadly may be treated by targeted inhibition of the FA/BRCA pathway.