Cell-Free DNA for Genomic Analysis in Primary Mediastinal Large B-Cell Lymphoma

Author:

Rivas-Delgado AlfredoORCID,Nadeu FerranORCID,Andrade-Campos Marcio,López CristinaORCID,Enjuanes AnnaORCID,Mozas PabloORCID,Frigola GerardORCID,Colomo LuisORCID,Sanchez-Gonzalez Blanca,Villamor Neus,Beà SílviaORCID,Campo Elías,Salar AntonioORCID,Giné Eva,López-Guillermo Armando,Bellosillo BeatrizORCID

Abstract

High-throughput sequencing of cell-free DNA (cfDNA) has emerged as a promising noninvasive approach in lymphomas, being particularly useful when a biopsy specimen is not available for molecular analysis, as it frequently occurs in primary mediastinal large B-cell lymphoma (PMBL). We used cfDNA for genomic characterization in 20 PMBL patients by means of a custom NGS panel for gene mutations and low-pass whole-genome sequencing (WGS) for copy number analysis (CNA) in a real-life setting. Appropriate cfDNA to perform the analyses was obtained in 18/20 cases. The sensitivity of cfDNA to detect the mutations present in paired FFPE samples was 69% (95% CI: 60–78%). The mutational landscape found in cfDNA samples was highly consistent with that of the tissue, with the most frequently mutated genes being B2M (61%), SOCS1 (61%), GNA13 (44%), STAT6 (44%), NFKBIA (39%), ITPKB (33%), and NFKBIE (33%). Overall, we observed a 75% concordance to detect CNA gains/losses between DNA microarray and low-pass WGS. The sensitivity of low-pass WGS was remarkably higher for clonal CNA (18/20, 90%) compared to subclonal alterations identified by DNA microarray. No significant associations between cfDNA amount and tumor burden or outcome were found. cfDNA is an excellent alternative source for the accurate genetic characterization of PMBL cases.

Funder

Instituto de Salud Carlos III

Centro de Investigación Biomédica en Red de Cáncer

European Union

European Hematology Association

American Association For Cancer Research

Lady Tata Memorial Trust

Government of Catalonia

Publisher

MDPI AG

Subject

Clinical Biochemistry

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