| Literature DB >> 26106858 |
Sonia A Melo1, Linda B Luecke1, Christoph Kahlert1, Agustin F Fernandez2, Seth T Gammon3, Judith Kaye1, Valerie S LeBleu1, Elizabeth A Mittendorf4, Juergen Weitz5, Nuh Rahbari5, Christoph Reissfelder5, Christian Pilarsky5, Mario F Fraga6, David Piwnica-Worms3, Raghu Kalluri1.
Abstract
Exosomes are lipid-bilayer-enclosed extracellular vesicles that contain proteins and nucleic acids. They are secreted by all cells and circulate in the blood. Specific detection and isolation of cancer-cell-derived exosomes in the circulation is currently lacking. Using mass spectrometry analyses, we identify a cell surface proteoglycan, glypican-1 (GPC1), specifically enriched on cancer-cell-derived exosomes. GPC1(+) circulating exosomes (crExos) were monitored and isolated using flow cytometry from the serum of patients and mice with cancer. GPC1(+) crExos were detected in the serum of patients with pancreatic cancer with absolute specificity and sensitivity, distinguishing healthy subjects and patients with a benign pancreatic disease from patients with early- and late-stage pancreatic cancer. Levels of GPC1(+) crExos correlate with tumour burden and the survival of pre- and post-surgical patients. GPC1(+) crExos from patients and from mice with spontaneous pancreatic tumours carry specific KRAS mutations, and reliably detect pancreatic intraepithelial lesions in mice despite negative signals by magnetic resonance imaging. GPC1(+) crExos may serve as a potential non-invasive diagnostic and screening tool to detect early stages of pancreatic cancer to facilitate possible curative surgical therapy.Entities:
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Year: 2015 PMID: 26106858 PMCID: PMC4825698 DOI: 10.1038/nature14581
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 69.504