Plasticity of circulating tumor cells in small cell lung cancer

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作者
Jiyoun Seo
Mihir Kumar
Jeremy Mason
Fiona Blackhall
Nicholas Matsumoto
Caroline Dive
James Hicks
Peter Kuhn
Stephanie N. Shishido
机构
[1] Michelson Center for Convergent Bioscience,Convergent Science Institute in Cancer
[2] University of Southern California,Institute of Urology, Catherine & Joseph Aresty Department of Urology
[3] Keck School of Medicine,Keck School of Medicine, Norris Comprehensive Cancer Center
[4] University of Southern California,Department of Medical Oncology
[5] University of Southern California,Cancer Research UK Lung Cancer Centre of Excellence
[6] The Christie NHS Foundation Trust,CRUK Manchester Institute Cancer Biomarker Centre
[7] University of Manchester and University College London,Department of Biological Sciences, Dornsife College of Letters, Arts, and Sciences
[8] University of Manchester,Department of Aerospace and Mechanical Engineering, Viterbi School of Engineering
[9] University of Southern California,Department of Biomedical Engineering, Viterbi School of Engineering
[10] University of Southern California,undefined
[11] University of Southern California,undefined
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摘要
Small cell lung cancer (SCLC) is an aggressive neuroendocrine tumor with low five-year survival rates. Recently described molecular phenotypes of SCLC exhibit differential vulnerabilities heralding potential for stratified treatment. Whilst tumor biopsy in SCLC is challenging, circulating tumor cells in the liquid biopsy are prevalent and can be repeatedly sampled accommodating the dynamic plasticity of SCLC phenotypes. The aim of this study was to characterize the heterogeneity of rare circulating cells with confirmed tumor origin and to explore a liquid biopsy approach for future clinical trials of targeted therapies. This study applied the 3rd generation of a previously validated direct imaging platform to 14 chemo-naive SCLC patients and 10 non-cancerous normal donor (ND) samples. Phenotypic heterogeneity of circulating rare cells in SCLC was observed and a patient-level classification model was established to stratify SCLC patients from non-cancerous donors. Eight rare cell groups, with combinations of epithelial, endothelial, and mesenchymal biomarker expression patterns, were phenotypically characterized. The single-cell genomic analysis confirmed the cancer cell plasticity in every rare cell group harboring clonal genomic alterations. This study shows rare cell heterogeneity and confirms cellular plasticity in SCLC providing a valuable resource for better opportunities to discover novel therapeutic targets in SCLC.
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