In this episode, Dr. Puri and Dr. Yu discuss how TP53 status informs first-line intensification in clinic. Both have moved to an opt-out approach: combination therapy is the default, and monotherapy is reserved for patients whose performance status, comorbidities, or preferences make combination unsuitable. Dr. Yu notes she had been intensifying selectively based on progression-free survival (PFS) data from FLAURA2 and MARIPOSA, but the overall survival (OS) readouts shifted her to upfront combination for nearly all patients. Dr. Puri agrees, noting the discussion in her clinic now starts with combination and works backward. They address the borderline patient — exon 19 deletion, low burden, no central nervous system (CNS) disease, but TP53 co-mutation — and conclude that risk factors are additive and even a single high-risk feature like TP53 generally tips the decision toward intensification. Roughly 60% of EGFR-mutant cases harbor TP53 alterations, so this is not a niche subgroup. On TP53 mutation type, Dr. Yu treats it as binary in practice while acknowledging truncating mutations confer worse prognosis than missense mutations. Dr. Puri notes that at Moffitt, paired tissue and liquid next-generation sequencing (NGS) often deliver TP53 results in time for first-line decisions, but she emphasizes that even without it, the opt-out strategy holds.
In the next episode, “Interpreting TOP Alongside FLAURA2 and MARIPOSA,” Dr. Yu and Dr. Puri compare the strength of evidence across the three intensification trials.