Proteogenomic characterization identifies clinical subgroups in EGFR and ALK wild-type never-smoker lung adenocarcinoma

Hyondeog Kim; Wonyeop Lee; Youngwook Kim; Sang-Jin Lee; Wonyoung Choi; Geon Kook Lee; Seung-Jin Park; Shinyeong Ju; Seon-Young Kim; Cheolju Lee; Ji-Youn Han

doi:10.1038/s12276-024-01320-0

Experimental and Molecular Medicine (Sep 2024)

Proteogenomic characterization identifies clinical subgroups in EGFR and ALK wild-type never-smoker lung adenocarcinoma

Hyondeog Kim,
Wonyeop Lee,
Youngwook Kim,
Sang-Jin Lee,
Wonyoung Choi,
Geon Kook Lee,
Seung-Jin Park,
Shinyeong Ju,
Seon-Young Kim,
Cheolju Lee,
Ji-Youn Han

Affiliations

Hyondeog Kim: Graduate School of Cancer Science and Policy, National Cancer Center
Wonyeop Lee: Anticancer Resistance Branch, Research Institute of National Cancer Center
Youngwook Kim: Graduate School of Cancer Science and Policy, National Cancer Center
Sang-Jin Lee: Immuno-oncology Branch, Research Institute of National Cancer Center
Wonyoung Choi: Cancer Molecular Biology Branch, Research Institute of National Cancer Center
Geon Kook Lee: Cancer Diagnostics Branch, Research Institute of National Cancer Center
Seung-Jin Park: Korea Research Institute of Bioscience and Biotechnology
Shinyeong Ju: Chemical & Biological Integrative Research Center, Korea Institute of Science and Technology
Seon-Young Kim: Korea Research Institute of Bioscience and Biotechnology
Cheolju Lee: Chemical & Biological Integrative Research Center, Korea Institute of Science and Technology
Ji-Youn Han: Anticancer Resistance Branch, Research Institute of National Cancer Center

DOI: https://doi.org/10.1038/s12276-024-01320-0
Journal volume & issue: Vol. 56, no. 9
pp. 2082 – 2095

Abstract

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Abstract Patients with lung adenocarcinoma who have never smoked (NSLA) and lack key driver mutations, such as those in the EGFR and ALK genes, face limited options for targeted therapies. They also tend to have poorer outcomes with immune checkpoint inhibitors than lung cancer patients who have a history of smoking. The proteogenomic profile of nonsmoking lung adenocarcinoma patients without these oncogenic driver mutations is poorly understood, which complicates the precise molecular classification of these cancers and highlights a significant area of unmet clinical need. This study analyzed the genome, transcriptome, and LC‒MS/MS-TMT-driven proteome data of tumors obtained from 99 Korean never-smoker lung adenocarcinoma patients. NSLA tumors without EGFR or ALK driver oncogenes were classified into four proteogenomic subgroups: proliferation, angiogenesis, immune, and metabolism subgroups. These 4 molecular subgroups were strongly associated with distinct clinical outcomes. The proliferation and angiogenesis subtypes were associated with a poorer prognosis, while the immune subtype was associated with the most favorable outcome, which was validated in an external lung cancer dataset. Genomic-wide impacts were analyzed, and significant correlations were found between copy number alterations and both the transcriptome and proteome for several genes, with enrichment in the ERBB, neurotrophin, insulin, and MAPK signaling pathways. Proteogenomic analyses suggested several targetable genes and proteins, including CDKs and ATR, as potential therapeutic targets in the proliferation subgroup. Upregulated cytokines, such as CCL5 and CXCL13, in the immune subgroup may serve as potential targets for combination immunotherapy. Our comprehensive proteogenomic analysis revealed the molecular subtypes of EGFR- and ALK-wild-type NSLA with significant unmet clinical needs.

Published in Experimental and Molecular Medicine

ISSN: 1226-3613 (Print); 2092-6413 (Online)
Publisher: Nature Publishing Group
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Chemistry: Organic chemistry: Biochemistry
Website: https://www.nature.com/emm/

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