Targeted Tissue and Cell-Free Tumor DNA Sequencing of Advanced Lung Squamous-Cell Carcinoma Reveals Clinically Significant Prevalence of Actionable Alterations

Overview

Journal Clin Lung Cancer

Publisher Elsevier

Specialties Oncology
Pulmonary Medicine

Date 2018 Oct 4

PMID 30279110

Citations 25

Authors

Vincent K Lam

Hai T Tran

Kimberly C Banks

Richard B Lanman

Waree Rinsurongkawong

Nir Peled

Jeff Lewis

J Jack Lee

Jack Roth

Emily B Roarty

Stephen Swisher

AmirAli Talasaz

P Andrew Futreal

Vassiliki Papadimitrakopoulou

John V Heymach

Jianjun Zhang

Affiliations

Soon will be listed here.

Abstract

Background: Major guidelines do not recommend routine molecular profiling of lung squamous-cell carcinoma (LUSC) because the prevalence of actionable alterations is thought to be low. Increased utilization of next-generation sequencing (NGS), particularly with cell-free circulating tumor DNA, facilitates reevaluation of this premise. PATIENTS AND METHODS: We retrospectively evaluated the prevalence of actionable alterations in 2 distinct LUSC cohorts totaling 492 patients. A total of 410 consecutive patients with stage 3B or 4 LUSC were tested with a targeted cell-free circulating DNA NGS assay, and 82 patients with LUSC of any stage were tested with a tissue NGS cancer panel.

Results: In the overall cohort, 467 patients (94.9%) had a diagnosis of LUSC, and 25 patients (5.1%) had mixed histology with a squamous component. A total of 10.5% of the LUSC subgroup had somatic alterations with therapeutic relevance, including in EGFR (2.8%), ALK/ROS1 (1.3%), BRAF (1.5%), and MET amplification or exon 14 skipping (5.1%). Sixteen percent of patients with mixed histology had an actionable alteration. In the LUSC subgroup, 3 evaluable patients were treated with targeted therapy for an actionable alteration; all of them experienced partial response.

Conclusion: In this large, real-world LUSC cohort, we observed a clinically significant prevalence of actionable alterations. Accurate local histopathologic assessment in advanced-stage LUSC can be challenging. Further evaluation of the genomic landscape in this setting is warranted to potentially identify underappreciated treatment options.

Citing Articles

Validity and utility of blood tumor mutational burden (bTMB) is dependent on circulating tumor DNA (ctDNA) shed: SCRUM-Japan MONSTAR-SCREEN.

Mishima S, Nakamura Y, Tukachinsky H, Taniguchi H, Kadowaki S, Kato K J Liq Biopsy. 2025; 1:100003.

PMID: 40027285 PMC: 11863975. DOI: 10.1016/j.jlb.2023.100003.

Case report: a case of lung squamous cell carcinoma with a novel FGFR3-IER5L fusion mutation responding to anlotinib.

Chen X, Zhao W, Yu H, Wang S, Wang C, Song Y Front Oncol. 2024; 14:1391349.

PMID: 39421453 PMC: 11484447. DOI: 10.3389/fonc.2024.1391349.

Non-small-cell lung cancer.

Hendriks L, Remon J, Faivre-Finn C, Garassino M, Heymach J, Kerr K Nat Rev Dis Primers. 2024; 10(1):71.

PMID: 39327441 DOI: 10.1038/s41572-024-00551-9.

Clinical Utility of Circulating Tumor DNA for Detecting Lung Cancer Mutations by Targeted Next-Generation Sequencing With Insufficient Tumor Samples.

Sun Y, Zhang X, Yang X, Ma J J Clin Lab Anal. 2024; 38(19-20):e25099.

PMID: 39315762 PMC: 11520943. DOI: 10.1002/jcla.25099.

Drug Response of Patient-Derived Lung Cancer Cells Predicts Clinical Outcomes of Targeted Therapy.

Kim S, Lee Y, Song B, Sim H, Kang E, Hwang M Cancers (Basel). 2024; 16(4).

PMID: 38398169 PMC: 10887363. DOI: 10.3390/cancers16040778.