The lateral displacement of cells orthogonal to a flow stream by rolling on asymmetrical receptor patterns presents a new opportunity for the label-free separation and analysis of cells. Understanding the nature of cell rolling trajectories on such substrates is necessary to the engineering of substrates and the design of devices for cell separation and analysis. Here, we investigate the statistical nature of cell rolling and the effect of pattern geometry and flow shear stress on cell rolling trajectories using micrometer-scale patterns of biomolecular receptors with well-defined edges. Leukemic myeloid HL60 cells expressing the PSGL-1 ligand were allowed to flow across a field of patterned lines fabricated using microcontact printing and functionalized with the P-selectin receptor, leveraging both the specific adhesion of this ligand−receptor pair and the asymmetry of the receptor pattern inclination angle with respect to the fluid shear flow direction (α = 5, 10, 15, and 20°). The effects of the fluid shear stress magnitude (τ = 0.5, 1, 1.5, and 2.0 dyn/cm[superscript 2]), α, and P-selectin incubation concentration were quantified in terms of the rolling velocity and edge tracking length. Rolling cells tracked along the inclined edges of the patterned lines before detaching and reattaching on another line. The detachment of rolling cells after tracking along the edge was consistent with a Poisson process of history-independent interactions. Increasing the edge inclination angle decreased the edge tracking length in an exponential manner, contrary to the shear stress magnitude and P-selectin incubation concentration, which did not have a significant effect. On the basis of these experimental data, we constructed an empirical model that predicted the occurrence of the maximum lateral displacement at an edge angle of 7.5°. We also used these findings to construct a Monte Carlo simulation for the prediction of rolling trajectories of HL60 cells on P-selectin-patterned substrates with a specified edge inclination angle. The prediction of lateral displacement in the range of 200 μm within a 1 cm separation length supports the feasibility of label-free cell separation via asymmetric receptor patterns in microfluidic devices.
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机译:通过在不对称受体图案上滚动,与流正交的细胞的横向位移为无标记的细胞分离和分析提供了新的机会。了解衬底上细胞滚动轨迹的性质对于衬底的工程设计以及用于细胞分离和分析的设备的设计是必不可少的。在这里,我们使用具有明确边缘的生物分子受体的微米尺度图案,研究细胞滚动的统计性质以及图案几何形状和流动剪切应力对细胞滚动轨迹的影响。表达PSGL-1配体的白血病髓样HL60细胞流经使用微接触印刷制造并使用P-选择素受体功能化的图案化线域,同时利用该配体-受体对的特异性粘附力和受体的不对称性相对于流体剪切流动方向的图案倾斜角(α= 5、10、15和20°)。根据轧制速度和边缘跟踪长度,量化了流体剪切应力强度(τ= 0.5、1、1.5和2.0 dyn / cm [上标2]),α和P-选择蛋白孵育浓度的影响。滚动单元沿图案线的倾斜边缘跟踪,然后分离并重新附着在另一条线上。沿边缘跟踪后滚动单元的分离与历史独立相互作用的泊松过程一致。与剪切应力大小和P-选择素孵育浓度相反,增加边缘倾斜角度以指数方式减少了边缘跟踪长度,但没有明显的作用。根据这些实验数据,我们构建了一个经验模型,该模型预测了在7.5°的边角处最大横向位移的发生。我们还利用这些发现构建了一个蒙特卡洛模拟,以预测具有指定边缘倾斜角的P-选择素图案底物上的HL60细胞的滚动轨迹。在1 cm分离长度内200μm范围内的横向位移的预测支持了通过微流体装置中的不对称受体模式进行无标记细胞分离的可行性。
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