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Microfluidic high-throughput encapsulation and hydrodynamic self-sorting of single cells

机译:单细胞微流高通量封装和流体动力自分选

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We present a purely hydrodynamic method for the high-throughput encapsulation of single cells into picoliter droplets, and spontaneous self-sorting of these droplets. Encapsulation uses a cell-triggered Rayleigh-Plateau instability in a flow-focusing geometry, and self-sorting puts to work two extra hydrodynamic mechanisms: lateral drift of deformable objects in a shear flow, and sterically driven dispersion in a compressional flow. Encapsulation and sorting are achieved on-flight in continuous flow at a rate up to 160 cells per second. The whole process is robust and cost-effective, involving no optical or electrical discrimination, active sorting, flow switching, or moving parts. Successful encapsulation and sorting of 70-80% of the injected cell population into drops containing one and only one cell, with <1% contamination by empty droplets, is demonstrated. The system is also applied to the direct encapsulation and sorting of cancerous lymphocytes from a whole blood mixture, yielding individually encapsulated cancer cells with a >10,000-fold enrichment as compared with the initial mix. The method can be implemented in simple "soft lithography" chips, allowing for easy downstream coupling with microfluidic cell biology or molecular biology protocols.
机译:我们提出了一种纯流体动力学方法,可将单个细胞高通量封装成皮升液滴,并自发地对这些液滴进行自动分选。封装在流动集中的几何形状中使用了由单元触发的瑞利高原不稳定性,而自分选则使两种额外的流体力学机制起作用:剪切流中可变形物体的横向漂移,以及压缩流中的空间驱动分散。封装和分选是在连续流中以高达160个细胞/秒的速度在飞行中实现的。整个过程坚固耐用且具有成本效益,不涉及光学或电气识别,主动分类,流量切换或移动部件。已证明成功地将70-80%的注射细胞群体封装和分选为包含一个和一个细胞的液滴,空液滴污染度小于1%。该系统还可用于从全血混合物中直接封装和分选癌细胞,从而获得单独封装的癌细胞,其富集度是初始混合物的10,000倍以上。该方法可以在简单的“软光刻”芯片中实施,从而允许与微流体细胞生物学或分子生物学方案的容易的下游偶联。

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