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Clinical application of whole-genome sequencing of solid tumors for precision oncology

Authors
Kim, R | Kim, S  | Oh, BB | Yu, WS  | Kim, CW  | Hur, H  | Son, SY  | Yang, MJ  | Cho, DS  | Ha, T  | Heo, S | Jang, JY  | Yun, JS  | Kwack, KS  | Kim, JK  | Huh, J  | Lim, SG  | Han, SU  | Lee, HW  | Park, JE  | Kim, CH  | Roh, J  | Koh, YW  | Lee, D  | Kim, JH  | Lee, GH  | Noh, CK  | Jung, YJ  | Park, JW  | Sheen, S  | Ahn, MS  | Choi, YW  | Kim, TH  | Kang, SY  | Choi, JH  | Baek, SY  | Lee, KM  | Kim, SI  | Noh, SH  | Kim, SH  | Hwang, H | Joo, E | Lee, S | Shin, JY | Yun, JY | Park, J | Yi, K | Kwon, Y | Lee, WC | Park, H | Lim, J | Yi, B | Koo, J | Koh, JY | Lee, S | Lee, Y | Lee, BR | Connolly-Strong, E | Ju, YS | Kwon, M
Citation
Experimental & molecular medicine, 56(8). : 1856-1868, 2024
Journal Title
Experimental & molecular medicine
ISSN
1226-36132092-6413
Abstract
Genomic alterations in tumors play a pivotal role in determining their clinical trajectory and responsiveness to treatment. Targeted panel sequencing (TPS) has served as a key clinical tool over the past decade, but advancements in sequencing costs and bioinformatics have now made whole-genome sequencing (WGS) a feasible single-assay approach for almost all cancer genomes in clinical settings. This paper reports on the findings of a prospective, single-center study exploring the real-world clinical utility of WGS (tumor and matched normal tissues) and has two primary objectives: (1) assessing actionability for therapeutic options and (2) providing clarity for clinical questions. Of the 120 patients with various solid cancers who were enrolled, 95 (79%) successfully received genomic reports within a median of 11 working days from sampling to reporting. Analysis of these 95 WGS reports revealed that 72% (68/95) yielded clinically relevant insights, with 69% (55/79) pertaining to therapeutic actionability and 81% (13/16) pertaining to clinical clarity. These benefits include the selection of informed therapeutics and/or active clinical trials based on the identification of driver mutations, tumor mutational burden (TMB) and mutational signatures, pathogenic germline variants that warrant genetic counseling, and information helpful for inferring cancer origin. Our findings highlight the potential of WGS as a comprehensive tool in precision oncology and suggests that it should be integrated into routine clinical practice to provide a complete image of the genomic landscape to enable tailored cancer management.
MeSH

DOI
10.1038/s12276-024-01288-x
PMID
39138315
Appears in Collections:
Journal Papers > School of Medicine / Graduate School of Medicine > Pathology
Journal Papers > School of Medicine / Graduate School of Medicine > Thoracic & Cardiovascular Surgery
Journal Papers > School of Medicine / Graduate School of Medicine > Surgery
Journal Papers > School of Medicine / Graduate School of Medicine > Gastroenterology
Journal Papers > School of Medicine / Graduate School of Medicine > Urology
Journal Papers > School of Medicine / Graduate School of Medicine > Radiology
Journal Papers > School of Medicine / Graduate School of Medicine > Otolaryngology
Journal Papers > School of Medicine / Graduate School of Medicine > Hematology-Oncology
Journal Papers > School of Medicine / Graduate School of Medicine > Pulmonary & Critical Care Medicine
Journal Papers > School of Medicine / Graduate School of Medicine > Neurosurgery
Ajou Authors
강, 석윤  |  고, 영화  |  곽, 규성  |  권, 민석  |  김, 석휘  |  김, 선일  |  김, 세혁  |  김, 장희  |  김, 재근  |  김, 창우  |  김, 철호  |  김, 태환  |  노, 성현  |  노, 진  |  노, 충균  |  박, 지원  |  박, 지은  |  백, 수연  |  손, 상용  |  신, 승수  |  안, 미선  |  양, 민재  |  유, 우식  |  윤, 재성  |  이, 기명  |  이, 길호  |  이, 다근  |  이, 현우  |  임, 선교  |  장, 전엽  |  정, 윤정  |  조, 대성  |  최, 용원  |  최, 진혁  |  하, 태양  |  한, 상욱  |  허, 지미  |  허, 훈
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