Analytical Performance of a Highly Sensitive System to Detect Gene Variants Using Next-Generation Sequencing for Lung Cancer Companion Diagnostics

Author:

Kato Kikuya1ORCID,Okami Jiro2,Nakamura Harumi3ORCID,Honma Keiichiro4ORCID,Sato Yoshiharu5,Nakamura Seiji1,Kukita Yoji13,Nakatsuka Shin-ichi4,Higashiyama Masahiko26

Affiliation:

1. Laboratory of Medical Genomics, Nara Institute of Science and Technology, Nara 630-0192, Japan

2. Department of General Thoracic Surgery, Osaka International Cancer Institute, Osaka 540-0008, Japan

3. Laboratory of Genomic Pathology, Osaka International Cancer Institute, Osaka 540-0008, Japan

4. Department of Diagnostic Pathology and Cytology, Osaka International Cancer Institute, Osaka 540-0008, Japan

5. DNA Chip Research Inc., Tokyo 105-0022, Japan

6. Department of Thoracic Surgery, Higashiosaka City Medical Center, Osaka 578-8588, Japan

Abstract

The recent increase in the number of molecular targeted agents for lung cancer has led to the demand for the simultaneous testing of multiple genes. Although gene panels using next-generation sequencing (NGS) are ideal, conventional panels require a high tumor content, and biopsy samples often do not meet this requirement. We developed a new NGS panel, called compact panel, characterized by high sensitivity, with detection limits for mutations of 0.14%, 0.20%, 0.48%, 0.24%, and 0.20% for EGFR exon 19 deletion, L858R, T790M, BRAF V600E, and KRAS G12C, respectively. Mutation detection also had a high quantitative ability, with correlation coefficients ranging from 0.966 to 0.992. The threshold for fusion detection was 1%. The panel exhibited good concordance with the approved tests. The identity rates were as follows: EGFR positive, 100% (95% confidence interval, 95.5–100); EGFR negative, 90.9 (82.2–96.3); BRAF positive, 100 (59.0–100); BRAF negative, 100 (94.9–100); KRAS G12C positive, 100 (92.7–100); KRAS G12C negative, 100 (93.0–100); ALK positive, 96.7 (83.8–99.9); ALK negative, 98.4 (97.2–99.2); ROS1 positive, 100 (66.4–100); ROS1 negative, 99.0 (94.6–100); MET positive, 98.0 (89.0–99.9); MET negative 100 (92.8–100); RET positive, 93.8 (69.8–100); RET negative, 100 (94.9–100). The analytical performance showed that the panel could handle various types of biopsy samples obtained by routine clinical practice without requiring strict pathological monitoring, as in the case of conventional NGS panels.

Publisher

MDPI AG

Subject

Clinical Biochemistry

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