Abstract 1408P
Background
Non-small cell lung cancer (NSCLC) can harbor different KRAS mutations. Although targeted therapy is available for KRAS G12C-mutant NSCLC, immune checkpoint inhibitors (ICIs) are still the first line treatment (tx) for these patients (pts). Here we aimed to assess the outcomes on ICIs for KRAS G12C compared to KRAS non-G12C-mutant pts.
Methods
This is an observational, retrospective, multicenter study in pts with KRAS-mutant NSCLC treated with ICIs (monotherapy or combination) between January 2017 and January 2023. Targeted sequencing was performed in most cases. Clinicopathological and molecular data were collected. We evaluated pts characteristics, tx response and survival outcomes from the beginning of ICIs in KRAS G12C vs non-G12C tumors.
Results
A total of 169 pts were included. NGS was performed in 105 pts, STK11 and TP53 were the most frequent co-mutated genes present in 4.4%/15% G12C/non-G12C (p=0.110) and 20%/35% G12C/non-G12C (p=0.143), respectively. There were no differences in median progression free survival (PFS) between G12C/non-G12C (8.8 vs 7.1 months(m) respectively p=0.727). In the multivariate analysis, PD-L1 negative tumors and ECOG ≥1 remained independently associated with worse PFS (p=0.010 and p= 0.002 respectively). Regarding overall survival (OS), harboring a G12C mutation was associated with a better OS compared with non-G12C tumors (mOS 16.2m vs 10.4m p=0.033), conversely PD-L1 negative tumors and basal ECOG of ≥1 was associated with worse OS (p= 0.002 and p<0.001 respectively).
Table: 1408P
Patient’s characteristics
N (%) | G12C (n=75) | Non-G12c (n=94) | p-value |
Median age | 62.9 | 63.8 | 0.471 |
Sex | 0.220 | ||
Male | 45 (60) | 66 (70.2) | |
Female | 30 (40) | 28 (29.7) | |
Tobacco | 0.203 | ||
Former | 34 (45.4) | 53 (56,4) | |
Current | 41 (54.6) | 41 (43.6) | |
Stage | 0.630 | ||
I-III | 17 (21.7) | 22 (23,4) | |
IV | 58 (78.3) | 72 (76.6) | |
M1 CNS | 14 (18.6) | 24 (25.5) | 0.381 |
M1 liver | 14 (18.6) | 20 (21.3) | 0.820 |
ICIs treatment line | 0.604 | ||
1 | 57 (76) | 75 (80) | |
≥2 | 18 (24) | 19 (20) | |
PD-L1 | 0.397 | ||
Negative (0%) | 17 (22.7) | 30 (32) | |
Positive (≥0%) | 58 (77.3) | 64 (68) | |
ECOG | 0.887 | ||
0 | 31 (41.4) | 41 (43.6) | |
≥1 | 44 (58.6) | 53 (56.4) |
Conclusions
Our work shows that patients with KRAS non-G12C tumors are more frequently PD-L1 negative and harbor a higher proportion of STK11 co-mutations conditioning a worse OS on immunotherapy treatment. Innovative therapeutic strategies need to be investigated for these patients.
Clinical trial identification
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
L. Masfarre Pinto: Other, Personal, Other, Travel Support: Kyowa Kirin. N. Castro Unanua: Financial Interests, Personal, Invited Speaker: Pierre Fabre; Financial Interests, Personal, Ownership Interest, Travel, congress registration: Merck, Roche; Financial Interests, Personal, Ownership Interest, Grant support: Expert Degree in Immuno-Oncology: Bristol Myers Squibb; Financial Interests, Personal, Ownership Interest, Travel: Pfizer. P. Rocha: Non-Financial Interests, Personal, Other, Travel Support: AstraZeneca. B. Bellosillo Paricio: Other, Personal, Other, Grant: Thermo Fisher, Roche Diagnostics, Roche Farma, AstraZeneca; Other, Personal, Other, Consultant: Amgen, AstraZeneca, Janssen, Novartis; Other, Personal, Speaker’s Bureau: Janssen, Merck-Serono, Novartis, Qiagen, Thermo Fisher, Pfizer, Bristol Myers Squibb. H. Arasanz: Other, Personal, Advisory Board: AstraZeneca; Other, Personal and Institutional, Other, Clinical Trial Coordination: Ferrer Farma; Other, Personal, Other, accommodation/travel expenses: Takeda, MSD, Angelini Farma. E. Arriola: Financial Interests, Personal, Advisory Board: Roche, Boehringer Ingelheim, Lilly; Financial Interests, Personal, Invited Speaker: Takeda, MSD, AstraZeneca, BMS, Thermo Fisher Scientific, Guardant Health, Pfizer; Financial Interests, Personal, Other, Co-founder: Trialing Health; Financial Interests, Institutional, Research Grant: AstraZeneca. All other authors have declared no conflicts of interest.
Resources from the same session
1443P - Patient-reported outcomes (PROs) with cemiplimab plus chemotherapy (CEMI + CHEMO) for first-line treatment of advanced non-small cell lung cancer (aNSCLC): PD-L1 level subgroups in EMPOWER-Lung 3
Presenter: Miranda Gogishvili
Session: Poster session 20
1444P - Sintilimab with two cycles nab-paclitaxel / platinum as first line therapy for advanced squamous non-small-cell lung cancer: The final analysis and biomarker results
Presenter: Huijuan Wang
Session: Poster session 20
1445P - A randomized phase III trial on Pembrolizumab Alone versUs pembrolizumab-chemotherapy in first LInE NSCLC (PAULIEN), results of the interim analysis
Presenter: Ilias Houda
Session: Poster session 20
1447P - IMscin001 part 2 updated results: Efficacy, safety, immunogenicity and patient-reported outcomes (PROs) from the randomised phase III study of atezolizumab (atezo) subcutaneous (SC) vs intravenous (IV) in patients with locally advanced or metastatic non-small cell lung cancer (NSCLC)
Presenter: Mauricio Burotto
Session: Poster session 20
1449P - The preliminary data from a single-arm, open-label, multicenter phase II clinical trial: KN046 combined with axitinib as first-line (1L) treatment for NSCLC
Presenter: Yuanyuan Zhao
Session: Poster session 20
1450P - Addition of bevacizumab to first-line chemoimmunotherapy in NSCLC with liver metastases
Presenter: Matthieu Roulleaux Dugage
Session: Poster session 20
1451P - Identifying long-term responders to immune checkpoint blockade: Potential utility of serum proteomic profiling in metastatic non-small cell lung cancer
Presenter: Rafael Bach Mora
Session: Poster session 20
1452P - Factors associated with real-world (rw) outcomes among pts with metastatic NSCLC (mNSCLC) receiving select immuno-oncology (IO) regimens: CORRELATE
Presenter: Stephen Liu
Session: Poster session 20