High-Sensitivity Mutation Analysis of Cell-Free DNA for Disease Monitoring in Endometrial Cancer

子宫内膜癌 医学 肿瘤科 内科学 癌症 胎儿游离DNA 阶段(地层学) 深度测序 DNA测序 疾病 基因 生物 遗传学 基因组 胎儿 古生物学 产前诊断 怀孕
作者
Charles Ashley,Pier Selenica,Juber Patel,Michelle Wu,Josip Ninčević,Yulia Lakhman,Qin Zhou,Ronak Shah,Michael F. Berger,Arnaud Da Cruz Paula,David Brown,Antonio Marra,Alexia Iasonos,Amir Momeni Boroujeni,Kaled M. Alektiar,Kara Long Roche,Oliver Zivanovic,Jennifer J. Mueller,Dmitriy Zamarin,Vance Broach
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:29 (2): 410-421 被引量:27
标识
DOI:10.1158/1078-0432.ccr-22-1134
摘要

Abstract Purpose: We sought to determine whether sequencing analysis of circulating cell-free DNA (cfDNA) in patients with prospectively accrued endometrial cancer captures the mutational repertoire of the primary lesion and allows for disease monitoring. Experimental Design: Peripheral blood was prospectively collected from 44 newly diagnosed patients with endometrial cancer over a 24-month period (i.e., baseline, postsurgery, every 6 months after). DNA from the primary endometrial cancers was subjected to targeted next-generation sequencing (NGS) of 468 cancer-related genes, and cfDNA to a high-depth NGS assay of 129 genes with molecular barcoding. Sequencing data were analyzed using validated bioinformatics methods. Results: cfDNA levels correlated with surgical stage in endometrial cancers, with higher levels of cfDNA being present in advanced-stage disease. Mutations in cfDNA at baseline were detected preoperatively in 8 of 36 (22%) patients with sequencing data, all of whom were diagnosed with advanced-stage disease, high tumor volume, and/or aggressive histologic type. Of the 38 somatic mutations identified in the primary tumors also present in the cfDNA assay, 35 (92%) and 38 (100%) were detected at baseline and follow-up, respectively. In 6 patients with recurrent disease, changes in circulating tumor DNA (ctDNA) fraction/variant allele fractions in cfDNA during follow-up closely mirrored disease progression and therapy response, with a lead time over clinically detected recurrence in two cases. The presence of ctDNA at baseline (P < 0.001) or postsurgery (P = 0.014) was significantly associated with reduced progression-free survival. Conclusions: cfDNA sequencing analysis in patients with endometrial cancer at diagnosis has prognostic value, and serial postsurgery cfDNA analysis enables disease and treatment response monitoring. See related commentary by Grant et al., p. 305

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