Current challenges for detection of circulating tumor cells and cell-free circulating nucleic acids, and their characterization in non-small cell lung carcinoma patients. What is the best blood substrate for personalized medicine?
Marius Ilie,Véronique Hofman,Elodie Long,Olivier Bordone,Eric Selva,Kevin Washetine,Charles-Hugo Marquette,Paul Hofman +7 more
TL;DR: The main advances in the field of CTC and ctDNA detection in NSCLC patients are described and the main advantages and disadvantages of these two approaches are compared.
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Abstract: The practice of “liquid biopsy” as a diagnostic, prognostic and theranostic tool in non-small cell lung cancer (NSCLC) patients is an appealing approach, at least in theory, since it is noninvasive and easily repeated. In particular, this approach allows patient monitoring during treatment, as well as the detection of different genomic alterations that are potentially accessible to targeted therapy or are associated with treatment resistance. However, clinical routine practice is slow to adopt the liquid biopsy. Several reasons may explain this: (I) the vast number of methods described for potential detection of circulating biomarkers, without a consensus on the ideal technical approach; (II) the multiplicity of potential biomarkers for evaluation, in particular, circulating tumor cells (CTCs) vs. circulating tumor DNA (ctDNA); (III) the difficulty in controlling the pre-analytical phase to obtain robust and reproducible results; (IV) the present cost of the currently available techniques, which limits accessibility to patients; (V) the turnaround time required to obtain results that are incompatible with the urgent need for delivery of treatment. The purpose of this review is to describe the main advances in the field of CTC and ctDNA detection in NSCLC patients and to compare the main advantages and disadvantages of these two approaches.
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Citations
Pros: Can tissue biopsy be replaced by liquid biopsy?
Marius Ilie,Paul Hofman +1 more
TL;DR: In the past decade, ‘personalized’ or ‘stratified’ management based on the molecular features of tumors of patients with advanced non-small-cell lung cancer has entered routine clinical practice, but faces several biological and technological challenges.
Detection of PD-L1 in circulating tumor cells and white blood cells from patients with advanced non-small-cell lung cancer
Marius Ilie,Edith Szafer-Glusman,Véronique Hofman,Emmanuel Chamorey,Salomé Lalvée,Eric Selva,Sylvie Leroy,C.-H. Marquette,Marcin Kowanetz,P. Hedge,Elizabeth Punnoose,Paul Hofman +11 more
TL;DR: Find a trend for worse survival in patients receiving first-line cisplatin-based chemotherapy treatments, whose tumors express PD-L1 in CTCs or immune cells (progression-free and overall survival), similar to the effects of PD- L1 expression in matched-patient tumors.
183
Enumeration and Molecular Characterization of Tumor Cells in Lung Cancer Patients Using a Novel In Vivo Device for Capturing Circulating Tumor Cells
Tobias M. Gorges,Nicole Penkalla,Thomas Schalk,Simon A. Joosse,Sabine Riethdorf,Johannes Tucholski,Klaus Lücke,Harriet Wikman,Stephen M. Jackson,Nora Brychta,Oliver von Ahsen,Christian Schumann,Thomas Krahn,Klaus Pantel +13 more
TL;DR: In vivo isolation of CTCs overcomes blood volume limitations of other approaches, which might help to implement CTC-based “liquid biopsies” into clinical decision making.
Clinical and biological significance of circulating tumor cells in cancer.
TL;DR: Markers from host cells, such as macrophages, mesenchymal stem cells, and bone marrow‐derived cells, which constitute the premetastatic niche, may become novel biomarkers for predicting relapse or metastasis or monitoring the effects of treatment.
141
Cell-free circulating tumor DNA in cancer
TL;DR: This review focuses on cell-free circulating tumor DNA in the bloodstream as a versatile biomarker that has the potential to accurately monitor tumor burden and treatment response, while also being able to monitor minimal residual disease, reducing the need for harmful adjuvant chemotherapy and allowing more rapid detection of relapse.
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