RAS signaling in lung adenocarcinoma is defined by lineage context and DUSP4 loss.
TL;DR
A novel EGFR mSig that captures the transcriptional footprint of EGFR activation revealed a subset of EGFR WT LUADs with "mt-like" features, which refines LUAD taxonomy beyond mutation-only pie-chart models by incorporating lineage and co-mutation context.
OpenAlex 토픽 ·
Protein Tyrosine Phosphatases
Protein Kinase Regulation and GTPase Signaling
Lung Cancer Treatments and Mutations
A novel EGFR mSig that captures the transcriptional footprint of EGFR activation revealed a subset of EGFR WT LUADs with "mt-like" features, which refines LUAD taxonomy beyond mutation-only pie-chart
APA
Minjeong Kim, Wisut Lamlertthon, et al. (2026). RAS signaling in lung adenocarcinoma is defined by lineage context and DUSP4 loss.. JCI insight, 11(8). https://doi.org/10.1172/jci.insight.200912
MLA
Minjeong Kim, et al.. "RAS signaling in lung adenocarcinoma is defined by lineage context and DUSP4 loss.." JCI insight, vol. 11, no. 8, 2026.
PMID
41817586
Abstract
BACKGROUNDThe molecular landscape of lung adenocarcinoma (LUAD) is often illustrated as a driver-oncogene pie chart, but identical mutations exhibit heterogeneous signaling shaped by comutations, transcriptional programs, and lineage context. We propose a lineage-integrated signaling framework using an EGFR mutation signature (mSig).METHODSWe defined EGFR mSig using differentially expressed genes in EGFR-mutant (EGFR-mt) LUADs. Semisupervised clustering and machine learning models were used to test reproducibility in different combinations of datasets. We analyzed molecular subtypes, lineage markers, co-occurring mutations, and EGFR copy number alterations in EGFR mSig-defined subtypes of LUAD.RESULTSEGFR mSig showed robust classification performance (area under receiver operating characteristic curve = 0.83-0.95; mean negative predictive value = 96.3%). Validated gene expression subtypes and lung lineage markers were closely aligned with EGFR mSig status. Most EGFR mSig+ tumors, including many without EGFR mutations, belonged to the bronchioid subtype. A subset of canonical RAS mutations were mSig+ and mirrored the EGFR mutation pattern. EGFR WT/mSig- tumors were enriched for nonbronchioid subtypes and had comutations in TP53 or RAS/RAF/RTKs. We highlight a parsimonious collection of coordinated mutations, including RAS, KEAP1, STK11, TP53, and CDKN2A, that taken together suggest coordination of tumor signaling previously suggested but now reproduced and expanded.CONCLUSIONA potentially novel EGFR mSig that captures the transcriptional footprint of EGFR activation revealed a subset of EGFR WT LUADs with mt-like features. mSig refines LUAD taxonomy beyond mutation-only pie-chart models by incorporating lineage and comutation context. Lineage-directed stratification with coalteration identifies clinically relevant groups across EGFR and RAS states and highlights treatment opportunities for patients currently considered oncogene-negative.FUNDINGNational Cancer Institute (NCI) U01CA272541, R01CA262296, U24CA264021, UG1CA233333, R01CA211939.
MeSH Terms
Humans; Adenocarcinoma of Lung; Lung Neoplasms; ErbB Receptors; Mutation; Signal Transduction; Dual-Specificity Phosphatases; Mitogen-Activated Protein Kinase Phosphatases; Gene Expression Regulation, Neoplastic; ras Proteins; Cell Lineage
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