A lab-on-a-disc platform enables serial monitoring of individual CTCs associated with tumor progression during EGFR-targeted therapy for patients with NSCLC
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Title
- A lab-on-a-disc platform enables serial monitoring of individual CTCs associated with tumor progression during EGFR-targeted therapy for patients with NSCLC
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Author(s)
- Minji Lim; Juhee Park; Alarice C. Lowe; Hyoung-oh Jeong; Semin Lee; Hee Chul Park; Kyusang Lee; Gwang Ha Kim; Mi-Hyun Kim; Yoon-Kyoung Cho
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Publication Date
- 2020-04
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Journal
- THERANOSTICS, v.10, no.12, pp.5181 - 5194
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Publisher
- IVYSPRING INT PUBL
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Abstract
- © The author(s). Rationale: Unlike traditional biopsy, liquid biopsy, which is a largely non-invasive diagnostic and monitoring tool, can be performed more frequently to better track tumors and mutations over time and to validate the efficiency of a cancer treatment. Circulating tumor cells (CTCs) are considered promising liquid biopsy biomarkers; however, their use in clinical settings is limited by high costs and a low throughput of standard platforms for CTC enumeration and analysis. In this study, we used a label-free, high-throughput method for CTC isolation directly from whole blood of patients using a standalone, clinical setting-friendly platform. Methods: A CTC-based liquid biopsy approach was used to examine the efficacy of therapy and emergent drug resistance via longitudinal monitoring of CTC counts, DNA mutations, and single-cell-level gene expression in a prospective cohort of 40 patients with epidermal growth factor receptor (EGFR)-mutant non-small cell lung cancer. Results: The change ratio of the CTC counts was associated with tumor response, detected by CT scan, while the baseline CTC counts did not show association with progression-free survival or overall survival. We achieved a 100% concordance rate for the detection of EGFR mutation, including emergence of T790M, between tumor tissue and CTCs. More importantly, our data revealed the importance of the analysis of the epithelial/mesenchymal signature of individual pretreatment CTCs to predict drug responsiveness in patients. Conclusion: The fluid-assisted separation technology disc platform enables serial monitoring of CTC counts, DNA mutations, as well as unbiased molecular characterization of individual CTCs associated with tumor progression during targeted therapy
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URI
- https://pr.ibs.re.kr/handle/8788114/8744
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DOI
- 10.7150/thno.44693
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ISSN
- 1838-7640
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Appears in Collections:
- Center for Soft and Living Matter(첨단연성물질 연구단) > 1. Journal Papers (저널논문)
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Items in DSpace are protected by copyright, with all rights reserved, unless otherwise indicated.