Clinical utility of the Oncomine Dx Target Test <scp>multi‐CDx</scp> system and the possibility of utilizing those original sequence data-Reference-Cited by-同舟云学术

Clinical utility of the Oncomine Dx Target Test multi‐CDx system and the possibility of utilizing those original sequence data

Published:2024-02 Issue:4 Volume:13 Page:
ISSN:2045-7634
Container-title:Cancer Medicine
language:en
Short-container-title:Cancer Medicine

Author:

Saito Ayaka¹,Terai Hideki¹²^ORCID,Kim Tae‐Jung³,Emoto Katsura⁴,Kawano Ryutaro⁵,Nakamura Kohei⁵^ORCID,Hayashi Hideyuki⁵,Takaoka Hatsuyo¹,Ogata Akihiko¹,Kinoshita Katsuhito¹,Ito Fumimaro¹,Shigematsu Lisa¹,Okada Masahiko¹,Fukushima Takahiro¹,Mitsuishi Akifumi¹,Shinozaki Taro¹,Ohgino Keiko¹,Ikemura Shinnosuke²⁶,Yasuda Hiroyuki¹,Kawada Ichiro¹⁷,Soejima Kenzo⁶⁸,Nishihara Hiroshi⁴,Fukunaga Koichi¹

Affiliation:

1. Department of Internal Medicine (Pulmonary Medicine), School of Medicine Keio University Tokyo Japan

2. Cancer Center, School of Medicine Keio University Tokyo Japan

3. Department of Hospital Pathology, Yeouido St. Mary Hospital, College of Medicine The Catholic University of Korea Seoul South Korea

4. Division of Diagnostic Pathology, School of Medicine Keio University Tokyo Japan

5. Genomics Unit, Keio Cancer Center, School of Medicine Keio University Tokyo Japan

6. Department of Respiratory Medicine, Graduate School of Medicine University of Yamanashi Yamanashi Japan

7. Keio University Health Center Keio University Tokyo Japan

8. Clinical Translational Research Center Keio University Hospital Tokyo Japan

Abstract

AbstractBackgroundCompanion diagnostic tests play a crucial role in guiding treatment decisions for patients with non‐small cell lung cancer (NSCLC). The Oncomine Dx Target Test (ODxTT) Multi‐CDx System has emerged as a prominent companion diagnostic method. However, its efficacy in detecting driver gene mutations, particularly rare mutations, warrants investigation.AimsThis study aimed to assess the performance of the ODxTT in detecting driver gene mutations in NSCLC patients. Specifically, we aimed to evaluate its sensitivity in detecting epidermal growth factor receptor (EGFR) mutations, a key determinant of treatment selection in NSCLC.Materials and MethodsWe conducted a retrospective analysis of NSCLC patients who underwent testing with the ODxTT at Keio University Hospital between May 2020 and March 2022. Patient samples were subjected to both DNA and RNA tests. Driver gene mutation status was assessed, and instances of missed mutations were meticulously examined.ResultsOf the 90 patients, five had nucleic acid quality problems, while 85 underwent both DNA and RNA tests. Driver gene mutations were detected in 56/90 (62.2%) patients. Of the 34 patient specimens, driver mutations were not detected using the ODxTT; however, epidermal growth factor receptor (EGFR) mutations were detected using polymerase chain reaction‐based testing in two patients, and a KRAS mutation was detected by careful examination of the sequence data obtained using the ODxTT in one patient. For the above three cases, carefully examining the gene sequence information obtained using the ODxTT could identify driver mutations that were not mentioned in the returned test results. Additionally, we confirmed comparable instances of overlook results for EGFR mutations in the dataset from South Korea, implying that this type of oversight could occur in other countries using the ODxTT. EGFR mutation was missed in ODxTT in Japan (6.3%, 2/32), South Korea (2.0%, 1/49), and overall (3.7%, 3/81).ConclusionEven if sufficient tumor samples are obtained, rare EGFR mutations (which are excluded from the ODxTT's genetic mutation list) might not be detected using the current ODxTT system due to the program used for sequence analysis. However, such rare EGFR mutations can still be accurately detected on ODxTT's sequence data using next‐generation sequencing.

Funder

MSD Life Science Foundation, Public Interest Incorporated Foundation

National Research Foundation of Korea

Japan Society for the Promotion of Science

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/cam4.7077

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