A novel strategy involves combining antibody-drug conjugates (ADCs) with PARP inhibitors. This approach could potentially overcome the need for a germline BRCA mutation, significantly broadening the patient population that could benefit from PARP inhibitor therapy in triple-negative breast cancer.
The TROPION-PanTumor01 study showed that patients who progressed on the TROP2-ADC sacituzumab govitecan still achieved responses to a second TROP2-ADC, Dato-DXD. This suggests that targeting the same antigen with a different payload can overcome initial resistance, informing future treatment sequencing.
The ADC Dato-DXD causes high rates of stomatitis and dry eye that are difficult to treat once they appear. Effective management requires aggressive, proactive prevention from the start of therapy using steroid mouthwash and lubricating eye drops, demanding significant patient engagement and vigilance.
The FDA is requiring higher US patient enrollment in global trials to address concerns that results from predominantly non-US populations (e.g., Asia) may not be generalizable. This reflects worries about differences in prior standard-of-care treatments and potential pharmacogenomic variations affecting outcomes.
The development of PARP-1 selective inhibitors like seriparib signals a shift in drug innovation. Instead of only chasing higher efficacy, these new agents aim for a more favorable toxicity profile (less GI toxicity, fewer dose discontinuations) to improve patient quality of life and treatment adherence.
The AscentO3 trial lacked an overall survival benefit for its primary endpoint because its design ethically allowed patients on the chemotherapy arm to receive sacituzumab govitecan upon progression. This 'crossover' improves care for the control group but makes it statistically difficult to demonstrate a first-line survival advantage.