Quantifying sequencing error and effective sequencing depth of liquid biopsy NGS with UMI error correction.
Malene Støchkel FrankJanina FußTim Alexander SteiertGreta VarkalaiteJulie GehlMichael ForsterPublished in: BioTechniques (2021)
Liquid biopsies are a minimally invasive method to diagnose and longitudinally monitor tumor mutations in patients when tissue biopsies are difficult (e.g., in lung cancer). The percentage of cell-free tumor DNA in blood plasma ranges from more than 65% to 0.1% or lower. To reliably diagnose tumor mutations at 0.1%, there are two options: unrealistically large volumes of patient blood or library preparation and sequencing depth optimized to low-input DNA. Here, we assess two library preparation methods and analysis workflows to determine feasibility and reliability based on standards with known allelic frequency (0 and 0.13% in PIK3CA). However, the implementation for patients is still costly and requires elaborate setups.
Keyphrases
- cell free
- end stage renal disease
- ejection fraction
- newly diagnosed
- minimally invasive
- chronic kidney disease
- healthcare
- circulating tumor
- single cell
- prognostic factors
- primary care
- peritoneal dialysis
- ultrasound guided
- case report
- ionic liquid
- optical coherence tomography
- fine needle aspiration
- robot assisted
- molecularly imprinted