Research paperLKB1/STK11 mutations in non-small cell lung cancer patients: Descriptive analysis and prognostic value

- LKB1/STK11 (STK11) is an onco-suppressor gene frequently inactivated in NSCLC.
- STK11 mutations were evaluated in a cohort largely enriched for advanced stages.
- STK11 and KRAS status were statistically associated.
- STK11 mutations did not impact upon patients' outcomes.
- A trend towards shorter survival was outlined for STK11 and KRAS co-mutated tumors.

BackgroundLKB1/STK11 (STK11) is among the most inactivated tumor-suppressor genes in non-small cell lung cancer (NSCLC). While evidence concerning the biologic role of STK11 is accumulating, its prognostic significance in advanced NSCLC has not been envisaged yet.Materials and methodsThis retrospective analysis included consecutive NSCLC patients with available STK11 information who underwent a platinum-based chemotherapy. STK11 mutational status was correlated to clinico-pathological and mutational features. Kaplan-Meier and Cox models were used for survival curves and multivariate analyses, respectively.ResultsAmong the 302 patients included, 267 (89%) were diagnosed with stage IIIB/IV NSCLC and 25 (8%) harbored a STK11 mutation (STK11mut). No statistical differences were observed between STK11 status and clinico-pathological variables. We detected a significant correlation between STK11 and KRAS status (p = 0.008); among the 25 STK11mut patients, 13 (52%) harbored a concomitant KRAS mutation. Overall survival (OS) was shorter for STK11mut (median OS = 10.4 months) compared to wild-type patients (STK11wt; median OS = 17.3 months) in univariate analysis (p = 0.085). STK11 status did not impact upon OS in multivariate analysis (p = 0.45) and non-significant results were observed for progression-free survival. The co-occurrence of KRAS and STK11 mutations suggest a trend toward detrimental effect in OS (p = 0.12).ConclusionsIn our cohort enriched for advanced NSCLC patients who received platinum-based chemotherapy, STK11 mutations were not specifically associated with clinico-pathological features and they did not impact upon survival. We confirm the positive correlation between STK11 and KRAS mutations. The co-occurrence of KRAS and STK11 mutations could label a more aggressive molecular subtype of NSCLC.