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Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications

Background: Liquid biopsies offer a promising alternative to tissue samples, providing non-invasive diagnostic approaches or serial monitoring of disease evolution. However, certain challenges remain, and the full potential of liquid biopsies has yet to be reached. Here we report several methodologi...

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Autores principales: Chudasama, Dimple, Katopodis, Periklis, Stone, Nick, Haskell, Jennifer, Sheridan, Hannah, Gardner, Benjamin, Urnovitz, Howard, Schuetz, Ekkehard, Beck, Julia, Hall, Marcia, Barr, James, Sisu, Cristina, Rice, Alexandra, Polychronis, Andreas, Anikin, Vladimir, Karteris, Emmanouil
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6468998/
https://www.ncbi.nlm.nih.gov/pubmed/30866571
http://dx.doi.org/10.3390/cancers11030331
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author Chudasama, Dimple
Katopodis, Periklis
Stone, Nick
Haskell, Jennifer
Sheridan, Hannah
Gardner, Benjamin
Urnovitz, Howard
Schuetz, Ekkehard
Beck, Julia
Hall, Marcia
Barr, James
Sisu, Cristina
Rice, Alexandra
Polychronis, Andreas
Anikin, Vladimir
Karteris, Emmanouil
author_facet Chudasama, Dimple
Katopodis, Periklis
Stone, Nick
Haskell, Jennifer
Sheridan, Hannah
Gardner, Benjamin
Urnovitz, Howard
Schuetz, Ekkehard
Beck, Julia
Hall, Marcia
Barr, James
Sisu, Cristina
Rice, Alexandra
Polychronis, Andreas
Anikin, Vladimir
Karteris, Emmanouil
author_sort Chudasama, Dimple
collection PubMed
description Background: Liquid biopsies offer a promising alternative to tissue samples, providing non-invasive diagnostic approaches or serial monitoring of disease evolution. However, certain challenges remain, and the full potential of liquid biopsies has yet to be reached. Here we report several methodological approaches to interrogate liquid biopsies using circulating tumour cell (CTC) enumeration and characterisation, transcriptomics, Raman spectroscopy, and copy number instability (CNI) scores using blood samples of lung cancer (LC) patients. Methods: We choose LC; since it still is the most common cause of cancer-related mortality worldwide, and therefore there is a need for development of new non-invasive diagnostic/prognostic technologies. Changes in gene expression were assessed using RNA-seq, and in CTCs using ImageStream, an imaging flow-cytometer. CNI scores, from paired tissue/ctDNA were also explored. Raman spectroscopy was used to provide chemical fingerprints of plasma samples. Results: CTCs were detected in all LC patients (n = 10). We observed a significant increase in CTC levels in LC patients (n = 10) compared to controls (n = 21). A similar CNI was noted in the tissue and plasma of 2 patients, where higher CNI scores corresponded with poorer outcome. Significant changes in Raman spectra (carotenoid concentrations) were noted in LC patients (n = 20) compared to controls (n = 10). RNA-seq revealed differential expression of 21 genes between LC cases and controls in both LC tissue and blood samples. Conclusions: Liquid biopsies can potentially provide a more comprehensive picture of the disease compared to a single tissue biopsy. CTC enumeration is feasible and sensitive for LC patients. Molecular profiling of CTCs is also possible from total blood. CNI scores and Raman spectra require further investigation. Further work is being undertaken to explore these methods of detection in a larger LC cohort.
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spelling pubmed-64689982019-04-23 Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications Chudasama, Dimple Katopodis, Periklis Stone, Nick Haskell, Jennifer Sheridan, Hannah Gardner, Benjamin Urnovitz, Howard Schuetz, Ekkehard Beck, Julia Hall, Marcia Barr, James Sisu, Cristina Rice, Alexandra Polychronis, Andreas Anikin, Vladimir Karteris, Emmanouil Cancers (Basel) Article Background: Liquid biopsies offer a promising alternative to tissue samples, providing non-invasive diagnostic approaches or serial monitoring of disease evolution. However, certain challenges remain, and the full potential of liquid biopsies has yet to be reached. Here we report several methodological approaches to interrogate liquid biopsies using circulating tumour cell (CTC) enumeration and characterisation, transcriptomics, Raman spectroscopy, and copy number instability (CNI) scores using blood samples of lung cancer (LC) patients. Methods: We choose LC; since it still is the most common cause of cancer-related mortality worldwide, and therefore there is a need for development of new non-invasive diagnostic/prognostic technologies. Changes in gene expression were assessed using RNA-seq, and in CTCs using ImageStream, an imaging flow-cytometer. CNI scores, from paired tissue/ctDNA were also explored. Raman spectroscopy was used to provide chemical fingerprints of plasma samples. Results: CTCs were detected in all LC patients (n = 10). We observed a significant increase in CTC levels in LC patients (n = 10) compared to controls (n = 21). A similar CNI was noted in the tissue and plasma of 2 patients, where higher CNI scores corresponded with poorer outcome. Significant changes in Raman spectra (carotenoid concentrations) were noted in LC patients (n = 20) compared to controls (n = 10). RNA-seq revealed differential expression of 21 genes between LC cases and controls in both LC tissue and blood samples. Conclusions: Liquid biopsies can potentially provide a more comprehensive picture of the disease compared to a single tissue biopsy. CTC enumeration is feasible and sensitive for LC patients. Molecular profiling of CTCs is also possible from total blood. CNI scores and Raman spectra require further investigation. Further work is being undertaken to explore these methods of detection in a larger LC cohort. MDPI 2019-03-07 /pmc/articles/PMC6468998/ /pubmed/30866571 http://dx.doi.org/10.3390/cancers11030331 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Chudasama, Dimple
Katopodis, Periklis
Stone, Nick
Haskell, Jennifer
Sheridan, Hannah
Gardner, Benjamin
Urnovitz, Howard
Schuetz, Ekkehard
Beck, Julia
Hall, Marcia
Barr, James
Sisu, Cristina
Rice, Alexandra
Polychronis, Andreas
Anikin, Vladimir
Karteris, Emmanouil
Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications
title Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications
title_full Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications
title_fullStr Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications
title_full_unstemmed Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications
title_short Liquid Biopsies in Lung Cancer: Four Emerging Technologies and Potential Clinical Applications
title_sort liquid biopsies in lung cancer: four emerging technologies and potential clinical applications
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6468998/
https://www.ncbi.nlm.nih.gov/pubmed/30866571
http://dx.doi.org/10.3390/cancers11030331
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