Despite strong single-agent trial results, experts believe the field is shifting away from continuous monotherapy. The most significant future impact for pirtobrutinib will likely be as a backbone of fixed-duration combination therapies with drugs like venetoclax, aiming for deeper remissions without indefinite treatment.
Pirtobrutinib's registrational trials used control arms (ibrutinib, bendamustine-rituximab) that are no longer the standard of care in the US. This strategy reflects the long timeline of trial design and the need to use comparators that are still considered a standard globally, ensuring broader regulatory acceptance and allowing for cross-trial comparisons.
Pirtobrutinib is the first BTK inhibitor to show a rate of atrial fibrillation equivalent to a chemoimmunotherapy control arm in a randomized trial. This uniquely safe cardiovascular profile makes it a strong first-line candidate for older Chronic Lymphocytic Leukemia (CLL) patients or those with significant heart-related comorbidities.
While pirtobrutinib works after covalent BTK inhibitors, no data shows covalent inhibitors work after pirtobrutinib failure. This uncertainty about future options makes clinicians cautious about using it as an initial therapy, especially for younger CLL patients who will need multiple treatments over their lifetime.
Even with positive results from two registrational Phase 3 trials, experts note a potential regulatory hurdle. The FDA has shown increasing concern over studies with a low proportion of patients from North America, a characteristic of these trials, potentially complicating an otherwise strong case for approval based on clinical merit.