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Single Cell Hydrodynamic Stretching and Microsieve Filtration Reveal Genetic Phenotypic and Treatment-Related Links to Cellular Deformability

机译:单细胞水力拉伸和微筛滤揭示了细胞变形的遗传表型和治疗相关的链接。

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摘要

Deformability is shown to correlate with the invasiveness and metastasis of cancer cells. Recent studies suggest epithelial-to-mesenchymal transition (EMT) might enable cancer metastasis. However, the correlation of EMT with cancer cell deformability has not been well elucidated. Cellular deformability could also help evaluate the drug response of cancer cells. Here, we combine hydrodynamic stretching and microsieve filtration to study cellular deformability in several cellular models. Hydrodynamic stretching uses extensional flow to rapidly quantify cellular deformability and size with high throughput at the single cell level. Microsieve filtration can rapidly estimate relative deformability in cellular populations. We show that colorectal cancer cell line RKO with the mesenchymal-like feature is more flexible than the epithelial-like HCT116. In another model, the breast epithelial cells MCF10A with deletion of the TP53 gene are also significantly more deformable compared to their isogenic wildtype counterpart, indicating a potential genetic link to cellular deformability. We also find that the drug docetaxel leads to an increase in the size of A549 lung cancer cells. The ability to associate mechanical properties of cancer cells with their phenotypes and genetics using single cell hydrodynamic stretching or the microsieve may help to deepen our understanding of the basic properties of cancer progression.
机译:显示出可变形性与癌细胞的侵袭性和转移相关。最近的研究表明,上皮到间质转化(EMT)可能使癌症转移。但是,EMT与癌细胞变形能力之间的相关性尚未得到很好的阐明。细胞可变形性也可以帮助评估癌细胞的药物反应。在这里,我们结合了流体动力学拉伸和微筛过滤来研究几种细胞模型中的细胞变形性。流体动力拉伸使用拉伸流动来快速量化细胞的可变形性和大小,并在单个细胞水平上以高通量进行。微筛过滤可以快速估计细胞群体中的相对可变形性。我们显示,具有间充质样特征的结直肠癌细胞系RKO比上皮样HCT116更具有弹性。在另一个模型中,与它们的同基因野生型对应物相比,具有TP53基因缺失的乳腺上皮细胞MCF10A也具有更大的可变形性,表明与细胞可变形性的潜在遗传联系。我们还发现多西他赛药物导致A549肺癌细胞的大小增加。使用单细胞流体动力学拉伸或微筛将癌细胞的机械特性与其表型和遗传学相关联的能力可能有助于加深我们对癌症进展的基本特性的了解。

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