While blinatumomab-TKI combinations avoid systemic chemotherapy toxicity, they are associated with higher rates of central nervous system (CNS) relapses. This necessitates an increased number of intrathecal chemotherapy doses to prevent CNS disease, a critical nuance for managing this 'simpler' approach.
The treatment backbone for Ph+ ALL is shifting away from intensive chemotherapy like hyper-CVAD. Chemotherapy-free regimens combining blinatumomab with a TKI (preferably ponatinib) are becoming the new standard, showing outcomes that are at least as good as, and likely better than, traditional chemotherapy.
A key nuance in managing ponatinib for Ph+ ALL is a response-adapted dosing strategy. Patients are typically started at a 30mg dose, which is then reduced to 15mg once a good minimal residual disease (MRD) response is achieved. This approach aims to maintain efficacy while mitigating long-term toxicity.
Despite the high likelihood (75%) of a T315I mutation at relapse on first or second-generation TKIs, testing is not critical for the immediate treatment decision. The most potent TKI, ponatinib, would be the next line of therapy regardless of the mutation status, making the test more of a confirmation than a decision driver.