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 micromixing 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.
Microfluidic isolation of platelet-covered circulating tumor cells.
利用微流控技术分离血小板包裹的循环肿瘤细胞
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作者:Jiang Xiaocheng, Wong Keith H K, Khankhel Aimal H, Zeinali Mahnaz, Reategui Eduardo, Phillips Matthew J, Luo Xi, Aceto Nicola, Fachin Fabio, Hoang Anh N, Kim Wooseok, Jensen Annie E, Sequist Lecia V, Maheswaran Shyamala, Haber Daniel A, Stott Shannon L, Toner Mehmet
| 期刊: | Lab on a Chip | 影响因子: | 5.400 |
| 时间: | 2017 | 起止号: | 2017 Oct 11; 17(20):3498-3503 |
| doi: | 10.1039/c7lc00654c | 研究方向: | 细胞生物学、肿瘤 |
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