Abstract
Introduction: The impact of TP53 co-mutations in EGFR mutated patients on PFS and OS is controversial. Different classifications of TP53 mutations with respect to functional and potential clinical impact have been published. Therefore, we retrospectively analyzed the impact of TP53 co-mutations on ORR, PFS and OS in a cohort of EGFR mutated NSCLC IV patients (UICC 7) using different classifications of TP53 mutations.Methods: 75 EGFR mutated NSCLC IV patients homogeneously treated with 1st line EGFR TKI were analyzed for TP53 co-mutations. TP53 mutations were classified according to three different types of classifications. The endpoints ORR, PFS and OS were investigated.Results: TP53 co-mutations were found in 29/59 patients (49.2%). TP53 co-mutations were a statistically significant independent negative predictive factor for ORR, PFS and OS. TP53 co-mutations were associated with inferior mPFS and mOS: mPFS/mOS 12 vs. 18/24 vs. 42 months for non-disruptive/disruptive mutations vs. WT (p < 0.004)/(p < 0.009), 11 vs. 17/23 vs. 42 months for pathogenic vs. non-pathogenic/WT (p < 0.001)/(p < 0.001), and 7 vs. 12 vs. 18/12 vs. 28 vs. 42 months for exon 8 vs. non-exon 8 vs. WT (p < 0.001)/(p < 0.002).Conclusions: TP53 co-mutations are frequent in EGFR mt+ NSCLC and have a strong negative impact on all clinical endpoints of TKI therapy.
Highlights
The impact of Tumor suppressor gene (TP53) co-mutations in Epidermal Growth Factor-Receptor (EGFR) mutated patients on Progression Free Survival (PFS) and Overall Survival (OS) is controversial
The standard of care of EGFR mutated patients is 1st line EGFR TKI treatment based on the results of a number of phase III trials showing a statistically significant advantage of EGFR TKI regarding Objective Response Rate (ORR), PFS (Progression Free Survival), toxicity and quality of life (QoL) as well as in some studies OS (Overall Survival) over chemotherapy [1, 2]
In EGFR mt+ Non-SmallCell Lung Cancer (NSCLC) patients the frequency of TP53 mutations ranges from 25.9% [4] and 41% [5] depending on the method of detection
Summary
The impact of TP53 co-mutations in EGFR mutated patients on PFS and OS is controversial. Different classifications of TP53 mutations with respect to functional and potential clinical impact have been published. We retrospectively analyzed the impact of TP53 co-mutations on ORR, PFS and OS in a cohort of EGFR mutated NSCLC IV patients (UICC 7) using different classifications of TP53 mutations. The standard of care of EGFR mutated patients is 1st line EGFR TKI treatment based on the results of a number of phase III trials showing a statistically significant advantage of EGFR TKI regarding ORR (objective response rate), PFS (Progression Free Survival), toxicity and quality of life (QoL) as well as in some studies OS (Overall Survival) over chemotherapy [1, 2]. TP53 co-mutations are observed in wild type (WT) NSCLC with an incidence of about 50% and have been associated with smoking status [3]. The impact of TP53 mutations on treatment outcome has not been definitively analysed in EGFR mt+ NSCLC
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