| Literature DB >> 31939681 |
Huu Thinh Nguyen1, Duc Huy Tran1, Quoc Dat Ngo2, Hong-Anh Thi Pham3,4, Thanh-Truong Tran3,4, Vu-Uyen Tran3,4, Truong-Vinh Ngoc Pham1, Trung Kien Le1, Ngoc-An Trinh Le1, Ngoc Mai Nguyen3,4, Binh Thanh Vo3,4, Luan Thanh Nguyen3,4, Thien-Chi Van Nguyen3,4, Quynh Tram Nguyen Bui3,4, Huu-Nguyen Nguyen3,4, Bac An Luong2, Linh Gia Hoang Le2, Duc Minh Do2, Thanh-Thuy Thi Do2,4, Anh Vu Hoang2, Kiet Truong Dinh4, Minh-Duy Phan3,5, Le Son Tran3, Hoa Giang3,4, Hoai-Nghia Nguyen2.
Abstract
The identification and quantification of actionable mutations are critical for guiding targeted therapy and monitoring drug response in colorectal cancer. Liquid biopsy (LB) based on plasma cell-free DNA analysis has emerged as a noninvasive approach with many clinical advantages over conventional tissue sampling. Here, we developed a LB protocol using ultra-deep massive parallel sequencing and validated its clinical performance for detection and quantification of actionable mutations in three major driver genes (KRAS, NRAS and BRAF). The assay showed a 92% concordance for mutation detection between plasma and paired tissues and great reliability in quantification of variant allele frequency.Entities:
Keywords: Liquid biopsy; actionable mutation; circulating tumor DNA; colorectal cancer; ultra-deep sequencing
Year: 2020 PMID: 31939681 DOI: 10.1080/07357907.2020.1713350
Source DB: PubMed Journal: Cancer Invest ISSN: 0735-7907 Impact factor: 2.176