Concordance between whole exome sequencing of circulating tumor DNA and tumor tissue

Author:

Leenanitikul JulaneeORCID,Chanchaem Prangwalai,Mankhong Suwanan,Denariyakoon Sikrit,Fongchaiya Valla,Arayataweegool Areeya,Angspatt Pattama,Wongchanapai Ploytuangporn,Prapanpoj Verayuth,Chatamra Kris,Pisitkun TrairakORCID,Sriswasdi SiraORCID,Wongkongkathep PiriyaORCID

Abstract

Next generation sequencing of circulating tumor DNA (ctDNA) has been used as a noninvasive alternative for cancer diagnosis and characterization of tumor mutational landscape. However, low ctDNA fraction and other factors can limit the ability of ctDNA analysis to capture tumor-specific and actionable variants. In this study, whole-exome sequencings (WES) were performed on paired ctDNA and tumor biopsy in 15 cancer patients to assess the extent of concordance between mutational profiles derived from the two source materials. We found that up to 16.4% ctDNA fraction can still be insufficient for detecting tumor-specific variants and that good concordance with tumor biopsy is consistently achieved at higher ctDNA fractions. Most importantly, ctDNA analysis can consistently capture tumor heterogeneity and detect key cancer-related genes even in a patient with both primary and metastatic tumors.

Funder

Chulalongkorn University

Faculty of Medicine, Chulalongkorn University

Publisher

Public Library of Science (PLoS)

Subject

Multidisciplinary

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