Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches

Cancers of unknown primary (CUPs) comprise a heterogeneous group of rare metastatic tumors whose primary site cannot be identified after extensive clinical–pathological investigations. CUP patients are generally treated with empirical chemotherapy and have dismal prognosis. As recently reported, CUP...

Descripción completa

Detalles Bibliográficos
Autores principales: Laprovitera, Noemi, Salamon, Irene, Gelsomino, Francesco, Porcellini, Elisa, Riefolo, Mattia, Garonzi, Marianna, Tononi, Paola, Valente, Sabrina, Sabbioni, Silvia, Fontana, Francesca, Manaresi, Nicolò, D’Errico, Antonia, Pantaleo, Maria A., Ardizzoni, Andrea, Ferracin, Manuela
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Cell and Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8222689/
https://www.ncbi.nlm.nih.gov/pubmed/34178989
http://dx.doi.org/10.3389/fcell.2021.666156
_version_ 1783711538818842624
author Laprovitera, Noemi
Salamon, Irene
Gelsomino, Francesco
Porcellini, Elisa
Riefolo, Mattia
Garonzi, Marianna
Tononi, Paola
Valente, Sabrina
Sabbioni, Silvia
Fontana, Francesca
Manaresi, Nicolò
D’Errico, Antonia
Pantaleo, Maria A.
Ardizzoni, Andrea
Ferracin, Manuela
author_facet Laprovitera, Noemi
Salamon, Irene
Gelsomino, Francesco
Porcellini, Elisa
Riefolo, Mattia
Garonzi, Marianna
Tononi, Paola
Valente, Sabrina
Sabbioni, Silvia
Fontana, Francesca
Manaresi, Nicolò
D’Errico, Antonia
Pantaleo, Maria A.
Ardizzoni, Andrea
Ferracin, Manuela
author_sort Laprovitera, Noemi
collection PubMed
description Cancers of unknown primary (CUPs) comprise a heterogeneous group of rare metastatic tumors whose primary site cannot be identified after extensive clinical–pathological investigations. CUP patients are generally treated with empirical chemotherapy and have dismal prognosis. As recently reported, CUP genome presents potentially druggable alterations for which targeted therapies could be proposed. The paucity of tumor tissue, as well as the difficult DNA testing and the lack of dedicated panels for target gene sequencing are further relevant limitations. Here, we propose that circulating tumor cells (CTCs) and circulating tumor DNA (ctDNA) could be used to identify actionable mutations in CUP patients. Blood was longitudinally collected from two CUP patients. CTCs were isolated with CELLSEARCH(®) and DEPArray(TM) NxT and Parsortix systems, immunophenotypically characterized and used for single-cell genomic characterization with Ampli1(TM) kits. Circulating cell-free DNA (ccfDNA), purified from plasma at different time points, was tested for tumor mutations with a CUP-dedicated, 92-gene custom panel using SureSelect Target Enrichment technology. In parallel, FFPE tumor tissue was analyzed with three different assays: FoundationOne CDx assay, DEPArray LibPrep and OncoSeek Panel, and the SureSelect custom panel. These approaches identified the same mutations, when the gene was covered by the panel, with the exception of an insertion in APC gene. which was detected by OncoSeek and SureSelect panels but not FoundationOne. FGFR2 and CCNE1 gene amplifications were detected in single CTCs, tumor tissue, and ccfDNAs in one patient. A somatic variant in ARID1A gene (p.R1276(∗)) was detected in the tumor tissue and ccfDNAs. The alterations were validated by Droplet Digital PCR in all ccfDNA samples collected during tumor evolution. CTCs from a second patient presented a pattern of recurrent amplifications in ASPM and SEPT9 genes and loss of FANCC. The 92-gene custom panel identified 16 non-synonymous somatic alterations in ccfDNA, including a deletion (I1485Rfs(∗)19) and a somatic mutation (p. A1487V) in ARID1A gene and a point mutation in FGFR2 gene (p.G384R). Our results support the feasibility of non-invasive liquid biopsy testing in CUP cases, either using ctDNA or CTCs, to identify CUP genetic alterations with broad NGS panels covering the most frequently mutated genes.
format Online
Article
Text
id pubmed-8222689
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-82226892021-06-25 Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches Laprovitera, Noemi Salamon, Irene Gelsomino, Francesco Porcellini, Elisa Riefolo, Mattia Garonzi, Marianna Tononi, Paola Valente, Sabrina Sabbioni, Silvia Fontana, Francesca Manaresi, Nicolò D’Errico, Antonia Pantaleo, Maria A. Ardizzoni, Andrea Ferracin, Manuela Front Cell Dev Biol Cell and Developmental Biology Cancers of unknown primary (CUPs) comprise a heterogeneous group of rare metastatic tumors whose primary site cannot be identified after extensive clinical–pathological investigations. CUP patients are generally treated with empirical chemotherapy and have dismal prognosis. As recently reported, CUP genome presents potentially druggable alterations for which targeted therapies could be proposed. The paucity of tumor tissue, as well as the difficult DNA testing and the lack of dedicated panels for target gene sequencing are further relevant limitations. Here, we propose that circulating tumor cells (CTCs) and circulating tumor DNA (ctDNA) could be used to identify actionable mutations in CUP patients. Blood was longitudinally collected from two CUP patients. CTCs were isolated with CELLSEARCH(®) and DEPArray(TM) NxT and Parsortix systems, immunophenotypically characterized and used for single-cell genomic characterization with Ampli1(TM) kits. Circulating cell-free DNA (ccfDNA), purified from plasma at different time points, was tested for tumor mutations with a CUP-dedicated, 92-gene custom panel using SureSelect Target Enrichment technology. In parallel, FFPE tumor tissue was analyzed with three different assays: FoundationOne CDx assay, DEPArray LibPrep and OncoSeek Panel, and the SureSelect custom panel. These approaches identified the same mutations, when the gene was covered by the panel, with the exception of an insertion in APC gene. which was detected by OncoSeek and SureSelect panels but not FoundationOne. FGFR2 and CCNE1 gene amplifications were detected in single CTCs, tumor tissue, and ccfDNAs in one patient. A somatic variant in ARID1A gene (p.R1276(∗)) was detected in the tumor tissue and ccfDNAs. The alterations were validated by Droplet Digital PCR in all ccfDNA samples collected during tumor evolution. CTCs from a second patient presented a pattern of recurrent amplifications in ASPM and SEPT9 genes and loss of FANCC. The 92-gene custom panel identified 16 non-synonymous somatic alterations in ccfDNA, including a deletion (I1485Rfs(∗)19) and a somatic mutation (p. A1487V) in ARID1A gene and a point mutation in FGFR2 gene (p.G384R). Our results support the feasibility of non-invasive liquid biopsy testing in CUP cases, either using ctDNA or CTCs, to identify CUP genetic alterations with broad NGS panels covering the most frequently mutated genes. Frontiers Media S.A. 2021-06-10 /pmc/articles/PMC8222689/ /pubmed/34178989 http://dx.doi.org/10.3389/fcell.2021.666156 Text en Copyright © 2021 Laprovitera, Salamon, Gelsomino, Porcellini, Riefolo, Garonzi, Tononi, Valente, Sabbioni, Fontana, Manaresi, D’Errico, Pantaleo, Ardizzoni and Ferracin. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cell and Developmental Biology
Laprovitera, Noemi
Salamon, Irene
Gelsomino, Francesco
Porcellini, Elisa
Riefolo, Mattia
Garonzi, Marianna
Tononi, Paola
Valente, Sabrina
Sabbioni, Silvia
Fontana, Francesca
Manaresi, Nicolò
D’Errico, Antonia
Pantaleo, Maria A.
Ardizzoni, Andrea
Ferracin, Manuela
Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches
title Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches
title_full Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches
title_fullStr Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches
title_full_unstemmed Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches
title_short Genetic Characterization of Cancer of Unknown Primary Using Liquid Biopsy Approaches
title_sort genetic characterization of cancer of unknown primary using liquid biopsy approaches
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8222689/
https://www.ncbi.nlm.nih.gov/pubmed/34178989
http://dx.doi.org/10.3389/fcell.2021.666156
work_keys_str_mv AT laproviteranoemi geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT salamonirene geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT gelsominofrancesco geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT porcellinielisa geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT riefolomattia geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT garonzimarianna geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT tononipaola geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT valentesabrina geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT sabbionisilvia geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT fontanafrancesca geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT manaresinicolo geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT derricoantonia geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT pantaleomariaa geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT ardizzoniandrea geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches
AT ferracinmanuela geneticcharacterizationofcancerofunknownprimaryusingliquidbiopsyapproaches

Ejemplares similares