Transcriptional subtypes of glottic cancer characterized by differential activation of canonical oncogenic programming

Author:

Panuganti Bharat A.123,Carico Christine3,Jeyarajan Harishanker13,Flagg Mitchell4,Tamayo Pablo45

Affiliation:

1. Department of Otolaryngology – Head and Neck Surgery The University of Alabama at Birmingham Birmingham Alabama USA

2. Birmingham Veteran Affairs Health Care System Birmingham Alabama USA

3. The University of Alabama at Birmingham School of Medicine Birmingham Alabama USA

4. University of California‐San Diego School of Medicine San Diego California USA

5. Moores Cancer Center, Center for Novel Therapeutics and Division of Genomics and Precision Medicine University of California‐San Diego School of Medicine San Diego California USA

Abstract

AbstractBackgroundThere is a paucity of data concerning molecular heterogeneity among glottic squamous cell carcinoma, and the clinical implications thereof.MethodsData corresponding to glottic squamous cell carcinoma were derived from The Cancer Genome Atlas. The Onco‐GPS computational methodology was levied to derive four patterns of transcriptional activity and three functional subtypes of glottic cancer.ResultsThirty glottic cancer samples stratified to three distinct oncogenic states (S0–S2) based on a Onco‐GPS model containing four transcriptional components (F0‐F3). Membership in S2 and association with transcriptional component F0 conveyed an invasive phenotype, with transcriptional activity strongly reflecting EMT programming (including TGF‐B and NF‐KB signaling). S2 membership also correlated with inferior disease‐specific survival (HR 9.027, 95% CI 1.021–79.767), and higher incidences of extracapsular spread and perineural invasion.ConclusionsWe present a functional taxonomy of glottic cancer, with subtypes demonstrating differential upregulation of canonical oncogenic networks and survival implications.

Funder

National Cancer Institute

Publisher

Wiley

Subject

Otorhinolaryngology

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