Issue 17, 2024

Efficient separation of large particles and giant cancer cells using an isosceles trapezoidal spiral microchannel

Abstract

Polyploid giant cancer cells (PGCCs) contribute to the genetic heterogeneity and evolutionary dynamics of tumors. Their size, however, complicates their isolation from mainstream tumor cell populations. Standard techniques like fluorescence-activated cell sorting (FACS) rely on fluorescent labeling, introducing potential challenges in subsequent PGCC analyses. In response, we developed the Isosceles Trapezoidal Spiral Microchannel (ITSμC), a microfluidic device optimizing the Dean drag force (FD) and exploiting uniform vortices for enhanced separation. Numerical simulations highlighted ITSμC's advantage in producing robust FD compared to rectangular and standard trapezoidal channels. Empirical results confirmed its ability to segregate larger polystyrene (PS) particles (avg. diameter: 50 μm) toward the inner wall, while directing smaller ones (avg. diameter: 23 μm) outward. Utilizing ITSμC, we efficiently isolated PGCCs from doxorubicin-resistant triple-negative breast cancer (DOXR-TNBC) and patient-derived cancer (PDC) cells, achieving outstanding purity, yield, and viability rates (all greater than 90%). This precision was accomplished without fluorescent markers, and the versatility of ITSμC suggests its potential in differentiating a wide range of heterogeneous cell populations.

Graphical abstract: Efficient separation of large particles and giant cancer cells using an isosceles trapezoidal spiral microchannel

Supplementary files

Article information

Article type
Paper
Submitted
27 May 2024
Accepted
21 Jul 2024
First published
22 Jul 2024

Analyst, 2024,149, 4496-4505

Efficient separation of large particles and giant cancer cells using an isosceles trapezoidal spiral microchannel

C. Park, W. Lim, R. Song, J. Han, D. You, S. Kim, J. E. Lee, D. van Noort, C. Mandenius, J. Lee, Kyung-A. Hyun, H. Jung and S. Park, Analyst, 2024, 149, 4496 DOI: 10.1039/D4AN00750F

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