Molecular profiling of single circulating tumor cells with diagnostic intention

Bernhard Polzer; Gianni Medoro; Sophie Pasch; Francesca Fontana; Laura Zorzino; Aurelia Pestka; Ulrich Andergassen; Franziska Meier‐Stiegen; Zbigniew T Czyz; Barbara Alberter; Steffi Treitschke; Thomas Schamberger; Maximilian Sergio; Giulia Bregola; Anna Doffini; Stefano Gianni; Alex Calanca; Giulio Signorini; Chiara Bolognesi; Arndt Hartmann; Peter A Fasching; Maria T Sandri; Brigitte Rack; Tanja Fehm; Giuseppe Giorgini; Nicolò Manaresi; Christoph A Klein

doi:10.15252/emmm.201404033

EMBO Molecular Medicine (Oct 2014)

Molecular profiling of single circulating tumor cells with diagnostic intention

Bernhard Polzer,
Gianni Medoro,
Sophie Pasch,
Francesca Fontana,
Laura Zorzino,
Aurelia Pestka,
Ulrich Andergassen,
Franziska Meier‐Stiegen,
Zbigniew T Czyz,
Barbara Alberter,
Steffi Treitschke,
Thomas Schamberger,
Maximilian Sergio,
Giulia Bregola,
Anna Doffini,
Stefano Gianni,
Alex Calanca,
Giulio Signorini,
Chiara Bolognesi,
Arndt Hartmann,
Peter A Fasching,
Maria T Sandri,
Brigitte Rack,
Tanja Fehm,
Giuseppe Giorgini,
Nicolò Manaresi,
Christoph A Klein

Affiliations

Bernhard Polzer: Project Group “Personalized Tumor Therapy”, Fraunhofer Institute for Toxicology und Experimental Medicine
Gianni Medoro: Silicon Biosystems S.p.A.
Sophie Pasch: Experimental Medicine and Therapy Research, University of Regensburg
Francesca Fontana: Silicon Biosystems S.p.A.
Laura Zorzino: Division of Laboratory Medicine, European Institute of Oncology
Aurelia Pestka: Department of Gynecology and Obstetrics, University Munich
Ulrich Andergassen: Department of Gynecology and Obstetrics, University Munich
Franziska Meier‐Stiegen: Department of Gynecology and Obstetrics, University of Düsseldorf
Zbigniew T Czyz: Project Group “Personalized Tumor Therapy”, Fraunhofer Institute for Toxicology und Experimental Medicine
Barbara Alberter: Project Group “Personalized Tumor Therapy”, Fraunhofer Institute for Toxicology und Experimental Medicine
Steffi Treitschke: Project Group “Personalized Tumor Therapy”, Fraunhofer Institute for Toxicology und Experimental Medicine
Thomas Schamberger: Experimental Medicine and Therapy Research, University of Regensburg
Maximilian Sergio: Silicon Biosystems S.p.A.
Giulia Bregola: Silicon Biosystems S.p.A.
Anna Doffini: Silicon Biosystems S.p.A.
Stefano Gianni: Silicon Biosystems S.p.A.
Alex Calanca: Silicon Biosystems S.p.A.
Giulio Signorini: Silicon Biosystems S.p.A.
Chiara Bolognesi: Silicon Biosystems S.p.A.
Arndt Hartmann: Department of Pathology, University Erlangen
Peter A Fasching: Department of Gynecology and Obstetrics, University Erlangen
Maria T Sandri: Division of Laboratory Medicine, European Institute of Oncology
Brigitte Rack: Department of Gynecology and Obstetrics, University Munich
Tanja Fehm: Department of Gynecology and Obstetrics, University of Düsseldorf
Giuseppe Giorgini: Silicon Biosystems S.p.A.
Nicolò Manaresi: Silicon Biosystems S.p.A.
Christoph A Klein: Project Group “Personalized Tumor Therapy”, Fraunhofer Institute for Toxicology und Experimental Medicine

DOI: https://doi.org/10.15252/emmm.201404033
Journal volume & issue: Vol. 6, no. 11
pp. 1371 – 1386

Abstract

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Abstract Several hundred clinical trials currently explore the role of circulating tumor cell (CTC) analysis for therapy decisions, but assays are lacking for comprehensive molecular characterization of CTCs with diagnostic precision. We therefore combined a workflow for enrichment and isolation of pure CTCs with a non‐random whole genome amplification method for single cells and applied it to 510 single CTCs and 189 leukocytes of 66 CTC‐positive breast cancer patients. We defined a genome integrity index (GII) to identify single cells suited for molecular characterization by different molecular assays, such as diagnostic profiling of point mutations, gene amplifications and whole genomes of single cells. The reliability of > 90% for successful molecular analysis of high‐quality clinical samples selected by the GII enabled assessing the molecular heterogeneity of single CTCs of metastatic breast cancer patients. We readily identified genomic disparity of potentially high relevance between primary tumors and CTCs. Microheterogeneity analysis among individual CTCs uncovered pre‐existing cells resistant to ERBB2‐targeted therapies suggesting ongoing microevolution at late‐stage disease whose exploration may provide essential information for personalized treatment decisions and shed light into mechanisms of acquired drug resistance.

Published in EMBO Molecular Medicine

ISSN: 1757-4676 (Print); 1757-4684 (Online)
Publisher: Springer Nature
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General); Science: Biology (General): Genetics
Website: https://www.embopress.org/journal/17574684

About the journal

Abstract

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