ESMO Congress 2024 | OncologyPRO

Topics

Clinical Research; Tumour Immunology; Pathology/Molecular Biology; Translational Research; Molecular Oncology; Immunotherapy

Author affiliations

¹ Department Of Medicine And Surgery, Università Campus Bio-Medico di Roma, 00128 - Rome/IT
² Operative Research Unit Of Medical Oncology, Fondazione Policlinico Universitario Campus Bio-Medico, 00128 - Rome/IT
³ Hematology And Oncology Department, ASST Grande Ospedale Metropolitano Niguarda, 20162 - Milan/IT
⁴ Department Of Onco-hematology, Papardo Hospital, 98158 - Messina/IT
⁵ Cancer Medicine Department, Gustave Roussy, 94805 - Villejuif/FR
⁶ Phase 1 Unit, Fondazione Policlinico Universitario A. Gemelli IRCCS, 00168 - Rome/IT
⁷ Department Of Surgery And Cancer, Hammersmith Hospital Campus, Imperial College London, W12 0NN - London/GB
⁸ Comprehensive Cancer Center, Fondazione Policlinico Universitario Agostino Gemelli IRCCS, Università Cattolica del Sacro Cuore, 00168 - Rome/IT
⁹ Medical Oncology, San Giuseppe Moscati Hospital, 74100 - Taranto/IT
¹⁰ Medical Oncology, Azienda Ospedaliera San Giovanni Addolorata, 00184 - Rome/IT

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Abstract 1338P

Background

Several evidence indicates a link between TP53 mutations and response to ICI in patients with NSCLC with conflicting results. While TP53 missense mutations have been associated with anti-tumor immune response, mechanistic studies suggest an immune-suppressive role for TP53 loss.

Methods

Patients with advanced, non-oncogene addicted NSCLC, treated with ICI-based regimens from Sep 2017 to Nov 2023 at 6 European institutions with available TP53 profiling were included. Patients were categorized as TP53 truncating (nonsense/frameshift), TP53 missense, TP53 others (splice sites, deletion), TP53 wild type. TP53 missense mutations were additionally screened through the GenomeNexus.org web tool. Clinical outcomes were overall survival (OS), real-world progression free survival (rwPFS). Data cut-off was March 2024.

Results

The final population consisted of 219 patients, mostly tested with F1DX1 (89%), of whom 81 (37.0%), 79 (36.1%), 43 (19.6%) and 16 (7.3%) were TP53 wt, TP53 missense, TP53 truncating and TP53 others. None of the baseline clinic-pathologic features was associated with the TP53 status, except for the increased PD-L1 expression, TMB and higher KRAS mutation rate reported for the TP53 missense group. The median FUP was 35.1 months. TP53 missense mutation was associated with a longer OS compared to TP53 truncating group (HR 0.62, 95%CI: 0.39-0.99) and longer PFS (HR 0.69, 95%CI: 0.49-0.97) compared to the TP53 wt group. In the multivariable analysis (including TMB, PD-L1, KRAS and STK11 and all available clinic-pathologic factors) confirmed that both TP53 wt (HR 0.58, 95%CI: 0.34-0.99) and TP53 missense (HR 0.49, 95%CI: 0.29-0.83) groups had a significantly decreased risk of death compared to TP53 truncating group, and that only the TP53 missense group had a significantly decreased risk of disease progression compared to both TP53 wt (HR 0.64, 95%CI: 0.42-0.95) and TP53 truncating (HR 0.56, 95CI%: 0.34-0.91) groups.

Conclusions

Our results highlight the heterogeneity linked to the TP53 mutational status, with tumors harbouring TP53 missense mutations possibly more immune-responsive than TP53 truncating/TP53 wt.

Poster session 05

1338P - TP53 truncating and missense mutations are linked to differential response to checkpoint blockade in patients with advanced non-small cell lung cancer (NSCLC)

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Abstract 1338P

Background

Methods

Results

Conclusions

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Funding

Disclosure

Abstract 1338P

Background

Methods

Results

Conclusions

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Funding

Disclosure

Resources from the same session