dc.contributor.author
Frost, Nikolaj
dc.contributor.author
Kollmeier, Jens
dc.contributor.author
Vollbrecht, Claudia
dc.contributor.author
Grah, Christian
dc.contributor.author
Matthes, Burkhard
dc.contributor.author
Pultermann, Dennis
dc.contributor.author
Laffert, Maximilian von
dc.contributor.author
Lüders, Heike
dc.contributor.author
Olive, Elisabeth
dc.contributor.author
Raspe, Matthias
dc.contributor.author
Mairinger, Thomas
dc.contributor.author
Ochsenreither, Sebastian
dc.contributor.author
Blum, Torsten
dc.contributor.author
Hummel, Michael
dc.contributor.author
Suttorp, Norbert
dc.contributor.author
Witzenrath, Martin
dc.contributor.author
Grohé, Christian
dc.date.accessioned
2021-05-12T12:48:43Z
dc.date.available
2021-05-12T12:48:43Z
dc.identifier.uri
https://refubium.fu-berlin.de/handle/fub188/30739
dc.identifier.uri
http://dx.doi.org/10.17169/refubium-30478
dc.description.abstract
Background: Pembrolizumab is a standard of care as first line palliative therapy in PD-L1 overexpressing (≥50%) non-small cell lung cancer (NSCLC). This study aimed at the identification of KRAS and TP53-defined mutational subgroups in the PD-L1 high population to distinguish long-term responders from those with limited benefit.
Methods: In this retrospective, observational study, patients from 4 certified lung cancer centers in Berlin, Germany, having received pembrolizumab monotherapy as first line palliative treatment for lung adenocarcinoma (LuAD) from 2017 to 2018, with PD-L1 expression status and targeted NGS data available, were evaluated.
Results: A total of 119 patients were included. Rates for KRAS, TP53 and combined mutations were 52.1%, 47.1% and 21.9%, respectively, with no association given between KRAS and TP53 mutations (P=0.24). By trend, PD-L1 expression was higher in KRAS-positive patients (75% vs. 65%, P=0.13). Objective response rate (ORR), median progression-free survival (PFS) and overall survival (OS) in the KRASG12C group (n=32, 51.6%) were 63.3%, 19.8 months (mo.) and not estimable (NE), respectively. Results in KRASother and wild type patients were similar and by far lower (42.7%, P=0.06; 6.2 mo., P<0.001; 23.4 mo., P=0.08). TP53 mutations alone had no impact on response and survival. However, KRASG12C/TP53 co-mutations (n=12) defined a subset of long-term responders (ORR 100.0%, PFS 33.3 mo., OS NE). In contrast, patients with KRASother/TP53 mutations showed a dismal prognosis (ORR 27.3%, P=0.002; PFS 3.9 mo., P=0.001, OS 9.7 mo., P=0.02).
Conclusions: A comprehensive assessment of KRAS subtypes and TP53 mutations allows a highly relevant prognostic differentiation of patients with metastatic, PD-L1 high LuAD treated upfront with pembrolizumab.
en
dc.rights.uri
https://creativecommons.org/licenses/by-nc-nd/4.0/
dc.subject
Non-small cell lung cancer (NSCLC)
en
dc.subject
checkpoint inhibitors
en
dc.subject
KRAS mutations
en
dc.subject
TP53 mutations
en
dc.subject.ddc
600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit
dc.title
KRASG12C/TP53 co-mutations identify long-term responders to first line palliative treatment with pembrolizumab monotherapy in PD-L1 high (≥50%) lung adenocarcinoma
dc.type
Wissenschaftlicher Artikel
dcterms.bibliographicCitation.doi
10.21037/tlcr-20-958
dcterms.bibliographicCitation.journaltitle
Translational Lung Cancer Research
dcterms.bibliographicCitation.number
2
dcterms.bibliographicCitation.originalpublishername
AME Publishing Company
dcterms.bibliographicCitation.pagestart
737
dcterms.bibliographicCitation.pageend
752
dcterms.bibliographicCitation.volume
10
refubium.affiliation
Charité - Universitätsmedizin Berlin
refubium.resourceType.isindependentpub
no
dcterms.accessRights.openaire
open access
dcterms.isPartOf.issn
2218-6751
dcterms.isPartOf.eissn
2226-4477