Nirmal K. Veeramachaneni scite author profile

BackgroundLung adenocarcinoma (LAD) has extreme genetic variation among patients, which is currently not well understood, limiting progress in therapy development and research. LAD intrinsic molecular subtypes are a validated stratification of naturally-occurring gene expression patterns and encompass different functional pathways and patient outcomes. Patients may have incurred different mutations and alterations that led to the different subtypes. We hypothesized that the LAD molecular subtypes co-occur with distinct mutations and alterations in patient tumors.Methodology/Principal FindingsThe LAD molecular subtypes (Bronchioid, Magnoid, and Squamoid) were tested for association with gene mutations and DNA copy number alterations using statistical methods and published cohorts (n = 504). A novel validation (n = 116) cohort was assayed and interrogated to confirm subtype-alteration associations. Gene mutation rates (EGFR, KRAS, STK11, TP53), chromosomal instability, regional copy number, and genomewide DNA methylation were significantly different among tumors of the molecular subtypes. Secondary analyses compared subtypes by integrated alterations and patient outcomes. Tumors having integrated alterations in the same gene associated with the subtypes, e.g. mutation, deletion and underexpression of STK11 with Magnoid, and mutation, amplification, and overexpression of EGFR with Bronchioid. The subtypes also associated with tumors having concurrent mutant genes, such as KRAS-STK11 with Magnoid. Patient overall survival, cisplatin plus vinorelbine therapy response and predicted gefitinib sensitivity were significantly different among the subtypes.Conclusions/ SignificanceThe lung adenocarcinoma intrinsic molecular subtypes co-occur with grossly distinct genomic alterations and with patient therapy response. These results advance the understanding of lung adenocarcinoma etiology and nominate patient subgroups for future evaluation of treatment response.

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Cost-effectiveness of routine mediastinoscopy in computed tomography– and positron emission tomography–screened patients with stage I lung cancer

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Siegel

et al. 2006

The Journal of Thoracic and Cardiovascular Surgery

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Management of Stage IIIA Non-Small Cell Lung Cancer by Thoracic Surgeons in North America

Veeramachaneni

Feins

Stephenson

et al. 2012

The Annals of Thoracic Surgery

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Local failure after complete resection of N0–1 non-small cell lung cancer

et al. 2011

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Risk factors for occult nodal metastasis in clinical T1N0 lung cancer: a negative impact on survival

Veeramachaneni

Battafarano

Meyers

et al. 2008

European Journal of Cardio-Thoracic Surgery

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