4.7 Article

Microfluidic isolation of platelet-covered circulating tumor cells

Journal

LAB ON A CHIP
Volume 17, Issue 20, Pages 3498-3503

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/c7lc00654c

Keywords

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Funding

  1. US National Institutes of Health (NIH) P41 BioMEMS Resource Center [EB002503]
  2. NIH National Institute of Biomedical Imaging and Bioengineering [EB012493]
  3. Howard Hughes Medical Institute
  4. American Cancer Society

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The interplay between platelets and tumor cells is known to play important roles in metastasis by enhancing tumor cell survival, tumor-vascular interactions, and escape from immune surveillance. However, platelet-covered circulating tumor cells (CTC) are extremely difficult to isolate due to masking or downregulation of surface epitopes. Here we describe a microfluidic platform that takes advantage of the satellite platelets on the surface of these stealth CTCs as a ubiquitous surface marker for isolation. Compared to conventional CTC enrichment techniques which rely on known surface markers expressed by tumor cells, platelet-targeted isolation is generally applicable to CTCs of both epithelial and mesenchymal phenotypes. Our approach first depletes unbound, free platelets by means of hydrodynamic size-based sorting, followed by immunoaffinity-based capture of platelet-covered CTCs using a herringbone micro-mixing device. This method enabled the reliable isolation of CTCs from 66% of lung and 60% of breast cancer (both epithelial) patient samples, as well as in 83% of melanoma (mesenchymal) samples. Interestingly, we observed special populations of CTCs that were extensively covered by platelets, as well as CTC-leukocyte clusters. Because these cloaked CTCs often escape conventional positive and negative isolation mechanisms, further characterization of these cells may uncover important yet overlooked biological information in blood-borne metastasis and cancer immunology.

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