Cell of origin markers identify different prognostic subgroups of lung adenocarcinoma

6533b7ddfe1ef96bd1275579

RESEARCH PRODUCT

Cell of origin markers identify different prognostic subgroups of lung adenocarcinoma

Giovannino Ciccone Francesca Maletta Anna Sapino Pier Luigi Filosso Nicola Veronese Francesco Guerrera Alberto Oliaro Fabrizio Tabbò Fabrizio Tabbò Marcello Gaudiano Claudio Luchini Enrico Ruffini Giorgio Inghirami Giorgio Inghirami Giorgio Inghirami Luisa Delsedime Licia Montagna Filomena Di Giacomo Filomena Di Giacomo Alessia Nottegar Aldo Scarpa Marco Chilosi Enrica Migliore

subject

Lung adenocarcinoma Morphology Adult Male 0301 basic medicine Oncology Biomarkers; Genetic mutations; Immunohistochemistry; Lung adenocarcinoma; Morphology; Survival analysis Pathology medicine.medical_specialty Candidate gene Cell of origin six-immunohistochemical markers panel (TTF1 SP-A Napsin A MUC5AC CDX2 and CK5)Adenocarcinoma of Lung Kaplan-Meier Estimate genetic mutations Gene mutation Biology medicine.disease_cause adenocarcinoma (ADC)survival analysis Pathology and Forensic Medicine 03 medical and health sciences 0302 clinical medicine Internal medicine morphology Biomarkers Tumor medicine Humans CDX2 Survival analysis Aged biomarkers; genetic mutations; immunohistochemistry; lung adenocarcinoma; morphology; survival analysis biomarkers Survival analysis Middle Aged respiratory system Prognosis lung adenocarcinoma medicine.disease Immunohistochemistry Genetic mutations 030104 developmental biology 030220 oncology & carcinogenesis immunohistochemistry Adenocarcinoma Immunohistochemistry Female KRAS Biomarkers

description

Strong prognostic markers able to stratify lung adenocarcinoma (ADC) patients are lacking. We evaluated whether a six-immunohistochemical markers panel (TTF1, SP-A, Napsin A, MUC5AC, CDX2 and CK5), defining the putative neoplastic “cell of origin,” allows to identify prognostic subgroups among lung ADC. We screened a large cohort of ADC specimens (2003–2013) from Torino Institutional Repository identifying: (i) marker positivity by immunohistochemistry, (ii) main morphological appearance by light microscopy, (iii) presence of “hotspot” mutations of candidate genes by Sequenom technology. To evaluate possible predictors of survival and time to recurrence, uni- and multivariable-adjusted comparisons were performed. We identified 4 different subgroups: “alveolar,” “bronchiolar,” “mixed” and “null type." Alveolar-differentiated ADC were more common in young (P =.065), female (P =.083) patients, frequently harboring EGFR-mutated (P =.003) tumors with acinar pattern (P <.001). Bronchiolar-differentiated ADC were more associated with mucinous and solid pattern (P <.001), higher degree of vascular invasion (P =.01) and KRAS gene mutations (P =.07). Bronchiolar, mixed, and null types were independent negative predictors for overall survival, and the latter two had a shorter time to recurrence. This “Cell of Origin” classifier is more predictable than morphology and genetics and is an independent predictor of survival on a multivariate analysis. © 2018 Elsevier Inc.

year	journal	country	edition	language
2018-01-01	Human Pathology

https://doi.org/10.1016/j.humpath.2018.01.017