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Massively-Parallelized, Deterministic Mechanoporation for Intracellular Delivery

机译:用于细胞内递送的大规模并行化,确定性机械镜

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Microfluidic intracellular delivery approaches based on plasma membrane poration have shown promise for addressing the limitations of conventional cellular engineering techniques in a wide range of applications in biology and medicine. However, the inherent stochasticity of the poration process in many of these approaches often results in a trade-off between delivery efficiency and cellular viability, thus potentially limiting their utility. Herein, we present a novel microfluidic device concept that mitigates this trade-off by providing opportunity for deterministic mechanoporation (DMP) of cells en masse. This is achieved by the impingement of each cell upon a single needle-like penetrator during aspiration-based capture, followed by diffusive influx of exogenous cargo through the resulting membrane pore, once the cells are released by reversal of flow. Massive parallelization enables high throughput operation, while single-site poration allows for delivery of small and large-molecule cargos in difficult-to-transfect cells with efficiencies and viabilities that exceed both conventional and emerging transfection techniques. As such, DMP shows promise for advancing cellular engineering practice in general and engineered cell product manufacturing in particular.
机译:基于血浆膜泡的微流体细胞内递送方法表明了解决常规蜂窝工程技术在各种生物学和医学应用中的局限性。然而,许多这些方法中的堆积过程的固有随机性经常导致输送效率和蜂窝活力之间的折衷,因此可能限制其效用。这里,我们提出了一种新的微流体装置概念,通过为细胞enmasse的确定性机械浴(DMP)提供机会来减轻该权衡。这是通过在基于抽吸的捕获过程中在单个针状穿透器时冲击每个细胞,然后通过所得膜孔的外源性货物的扩散流入,一旦通过逆转流动释放细胞。巨大的并行化能够实现高通量运算,而单点化液允许在难以转染的细胞中递送小型和大分子尸体,其具有超过常规和新出现的转染技术的效率和能力。因此,DMP尤其显示了在一般和工程电池产品制造中推进蜂窝工程实践的承诺。

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