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Elucidating acquired PARP inhibitor resistance in advanced prostate cancer.


ABSTRACT: PARP inhibition (PARPi) has anti-tumor activity against castration-resistant prostate cancer (CRPC) with homologous recombination repair (HRR) defects. However, mechanisms underlying PARPi resistance are not fully understood. While acquired mutations restoring BRCA genes are well documented, their clinical relevance, frequency, and mechanism of generation remain unclear. Moreover, how resistance emerges in BRCA2 homozygously deleted (HomDel) CRPC is unknown. Evaluating samples from patients with metastatic CRPC treated in the TOPARP-B trial, we identify reversion mutations in most BRCA2/PALB2-mutated tumors (79%) by end of treatment. Among reversions mediated by frameshift deletions, 60% are flanked by DNA microhomologies, implicating POLQ-mediated repair. The number of reversions and time of their detection associate with radiological progression-free survival and overall survival (p < 0.01). For BRCA2 HomDels, selection for rare subclones without BRCA2-HomDel is observed following PARPi, confirmed by single circulating-tumor-cell genomics, biopsy fluorescence in situ hybridization (FISH), and RNAish. These data support the need for restored HRR function in PARPi resistance.

SUBMITTER: Seed G 

PROVIDER: S-EPMC7618010 | biostudies-literature | 2024 Dec

REPOSITORIES: biostudies-literature

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Elucidating acquired PARP inhibitor resistance in advanced prostate cancer.

Seed George G   Beije Nick N   Yuan Wei W   Bertan Claudia C   Goodall Jane J   Lundberg Arian A   Tyler Matthew M   Figueiredo Ines I   Pereira Rita R   Baker Chloe C   Bogdan Denisa D   Gallagher Lewis L   Cieslik Jan-Phillipp JP   Greening Semini S   Lambros Maryou M   Neves Rui R   Magraner-Pardo Lorena L   Fowler Gemma G   Ebbs Berni B   Miranda Susana S   Flohr Penny P   Bianchini Diletta D   Rescigno Pasquale P   Porta Nuria N   Hall Emma E   Gurel Bora B   Tunariu Nina N   Sharp Adam A   Pettit Stephen S   Stoecklein Nikolas H NH   Sandhu Shahneen S   Quigley David D   Lord Christopher J CJ   Mateo Joaquin J   Carreira Suzanne S   de Bono Johann J  

Cancer cell 20241121 12


PARP inhibition (PARPi) has anti-tumor activity against castration-resistant prostate cancer (CRPC) with homologous recombination repair (HRR) defects. However, mechanisms underlying PARPi resistance are not fully understood. While acquired mutations restoring BRCA genes are well documented, their clinical relevance, frequency, and mechanism of generation remain unclear. Moreover, how resistance emerges in BRCA2 homozygously deleted (HomDel) CRPC is unknown. Evaluating samples from patients with  ...[more]

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