MFast-SeqS As a Monitoring and Pre-screening Tool for Tumor-Specific Aneuploidy in Plasma DNA

Overview

Journal Adv Exp Med Biol

Specialties Biology
General Medicine

Date 2016 Oct 19

PMID 27753036

Citations 14

Authors

Jelena Belic

Marina Koch

Peter Ulz

Martina Auer

Teresa Gerhalter

Sumitra Mohan

Katja Fischereder

Edgar Petru

Thomas Bauernhofer

Jochen B Geigl

Michael R Speicher

Ellen Heitzer

Affiliations

Soon will be listed here.

Abstract

Recent progress in the analysis of cell-free DNA fragments (cell-free circulating tumor DNA, ctDNA) now allows monitoring of tumor genomes by non-invasive means. However, previous studies with plasma DNA from patients with cancer demonstrated highly variable allele frequencies of ctDNA. Comprehensive genome-wide analysis of tumor genomes is greatly facilitated when plasma DNA has increased amounts of ctDNA. In order to develop a fast and cost-effective pre-screening method for the identification of plasma samples suitable for further extensive qualitative analysis, we adapted the recently described FAST-SeqS method. We show that our modified FAST-SeqS method (mFAST-SeqS) can be used as a pre-screening tool for an estimation of the ctDNA percentage. Moreover, since the genome-wide mFAST-SeqS z-scores correlate with the actual tumor content in plasma samples, changes in ctDNA levels associated with response to treatment can be easily monitored without prior knowledge of the genetic composition of tumor samples.

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