Journal: Breast cancer research : BCR
This study evaluated 16 BRCA1 variants of uncertain significance (VUS) identified in a hereditary cancer genetic counseling setting. Researchers used two homologous recombination (HR) repair assays to assess the variants’ impact on DNA repair function.
Key findings include:
- Five VUS were classified as pathogenic due to significantly impaired HR efficiency.
- Eleven VUS were deemed benign.
- Two pathogenic variants were located outside known BRCA1 functional domains.
- Four of the pathogenic variants showed increased sensitivity to ionizing radiation.
- Two pathogenic variants also displayed hypersensitivity to the PARP inhibitor olaparib, indicating potential therapeutic implications.
The authors emphasize that HR-based functional assays, combined with sensitivity testing, provide timely and clinically relevant data. This approach aids in the classification of BRCA1 VUS for genetic counseling and personalized treatment decisions.