TY - JOUR
T1 - KRAS G12C-mutated advanced non-small cell lung cancer
T2 - A real-world cohort from the German prospective, observational, nation-wide CRISP Registry (AIO-TRK-0315)
AU - the CRISP Registry Group
AU - Sebastian, Martin
AU - Eberhardt, Wilfried E.E.
AU - Hoffknecht, Petra
AU - Metzenmacher, Martin
AU - Wehler, Thomas
AU - Kokowski, Konrad
AU - Alt, Jürgen
AU - Schütte, Wolfgang
AU - Büttner, Reinhard
AU - Heukamp, Lukas C.
AU - Stenzinger, Albrecht
AU - Jänicke, Martina
AU - Fleitz, Annette
AU - Zacharias, Stefan
AU - Dille, Stephanie
AU - Hipper, Annette
AU - Sandberg, Marlen
AU - Weichert, Wilko
AU - Groschek, Matthias
AU - von der Heyde, Eyck
AU - Rauh, Jacqueline
AU - Dechow, Tobias
AU - Thomas, Michael
AU - Griesinger, Frank
N1 - Publisher Copyright:
© 2021 The Author(s)
PY - 2021/4
Y1 - 2021/4
N2 - Objectives: After decades of unsuccessful efforts in inhibiting KRAS, promising clinical data targeting the mutation subtype G12C emerge. Since little is known about outcome with standard treatment of patients with G12C mutated non-small cell lung cancer (NSCLC), we analyzed a large, representative, real-world cohort from Germany. Patients and methods: A total of 1039 patients with advanced KRAS-mutant or -wildtype NSCLC without druggable alterations have been recruited in the prospective, observational registry CRISP from 12/2015 to 06/2019 by 98 centers in Germany. Details on treatment, best response, and outcome were analyzed for patients with KRAS wildtype, G12C, and non-G12C mutations. Results: Within the study population, 160 (15.4 %) patients presented with KRAS G12C, 251 (24.2 %) with non-G12C mutations, 628 (60.4 %) with KRAS wildtype. High PD-L1 expression (Tumor Proportion Score, TPS > 50 %) was documented for 28.0 %, 43.5 %, and 28.9 % (wildtype, G12C, non-G12C) of the tested patients; 68.8 %, 89.3 %, and 87.7 % of the patients received first-line treatment combined with an immune checkpoint-inhibitor in 2019. TPS > 50 % vs. TPS < 1 % was associated with a significantly decreased risk of mortality in a multivariate Cox model (HR 0.39, 95 % CI 0.26−0.60, p=<0.001). There were no differences in clinical outcome between KRAS wildtype, G12C or non-G12C mutations and KRAS mutational status was not prognostic in the model. Conclusion: Here we describe the so far largest prospectively recruited cohort of patients with advanced NSCLC and KRAS mutations, with special focus on the G12C mutation. These data constitute an extremely valuable historical control for upcoming clinical studies that employ KRAS inhibitors.
AB - Objectives: After decades of unsuccessful efforts in inhibiting KRAS, promising clinical data targeting the mutation subtype G12C emerge. Since little is known about outcome with standard treatment of patients with G12C mutated non-small cell lung cancer (NSCLC), we analyzed a large, representative, real-world cohort from Germany. Patients and methods: A total of 1039 patients with advanced KRAS-mutant or -wildtype NSCLC without druggable alterations have been recruited in the prospective, observational registry CRISP from 12/2015 to 06/2019 by 98 centers in Germany. Details on treatment, best response, and outcome were analyzed for patients with KRAS wildtype, G12C, and non-G12C mutations. Results: Within the study population, 160 (15.4 %) patients presented with KRAS G12C, 251 (24.2 %) with non-G12C mutations, 628 (60.4 %) with KRAS wildtype. High PD-L1 expression (Tumor Proportion Score, TPS > 50 %) was documented for 28.0 %, 43.5 %, and 28.9 % (wildtype, G12C, non-G12C) of the tested patients; 68.8 %, 89.3 %, and 87.7 % of the patients received first-line treatment combined with an immune checkpoint-inhibitor in 2019. TPS > 50 % vs. TPS < 1 % was associated with a significantly decreased risk of mortality in a multivariate Cox model (HR 0.39, 95 % CI 0.26−0.60, p=<0.001). There were no differences in clinical outcome between KRAS wildtype, G12C or non-G12C mutations and KRAS mutational status was not prognostic in the model. Conclusion: Here we describe the so far largest prospectively recruited cohort of patients with advanced NSCLC and KRAS mutations, with special focus on the G12C mutation. These data constitute an extremely valuable historical control for upcoming clinical studies that employ KRAS inhibitors.
KW - Cohort studies
KW - KRAS G12C mutation
KW - KRAS mutations
KW - Non-small cell lung cancer
KW - PD-L1 expression
UR - http://www.scopus.com/inward/record.url?scp=85100908806&partnerID=8YFLogxK
U2 - 10.1016/j.lungcan.2021.02.005
DO - 10.1016/j.lungcan.2021.02.005
M3 - Article
C2 - 33611226
AN - SCOPUS:85100908806
SN - 0169-5002
VL - 154
SP - 51
EP - 61
JO - Lung Cancer
JF - Lung Cancer
ER -