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Single-cell Migration Chip for Chemotaxis-based Microfluidic Selection of Heterogeneous Cell Populations

机译:用于趋化性基于趋化性微流体选择的单细胞迁移芯片的异质细胞群

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摘要

Tumor cell migration toward and intravasation into capillaries is an early and key event in cancer metastasis, yet not all cancer cells are imbued with the same capability to do so. This heterogeneity within a tumor is a fundamental property of cancer. Tools to help us understand what molecular characteristics allow a certain subpopulation of cells to spread from the primary tumor are thus critical for overcoming metastasis. Conventional in vitro migration platforms treat populations in aggregate, which leads to a masking of intrinsic differences among cells. Some migration assays reported recently have single-cell resolution, but these platforms do not provide for selective retrieval of the distinct migrating and non-migrating cell populations for further analysis. Thus, to study the intrinsic differences in cells responsible for chemotactic heterogeneity, we developed a single-cell migration platform so that individual cells’ migration behavior can be studied and the heterogeneous population sorted based upon chemotactic phenotype. Furthermore, after migration, the highly chemotactic and non-chemotactic cells were retrieved and proved viable for later molecular analysis of their differences. Moreover, we modified the migration channel to resemble lymphatic capillaries to better understand how certain cancer cells are able to move through geometrically confining spaces.
机译:肿瘤细胞迁移到毛细血管中是一种早期和关键事件在癌症转移中,但并非所有癌细胞都具有相同的能力。肿瘤内的这种异质性是癌症的基本性质。帮助我们了解分子特性允许某种细胞群从原发性肿瘤传播的分子特征因此对于克服转移至关重要。常规的体外迁移平台在聚集体中治疗群体,这导致细胞之间的内在差异掩盖。报告的一些迁移测定最近具有单细胞分辨率,但这些平台不提供不同迁移和非迁移细胞群的选择性检索以进行进一步分析。因此,为了研究负责趋化异质性的细胞的内在差异,我们开发了一种单细胞迁移平台,以便可以研究单个细胞的迁移行为,并且基于趋化表型分类的异质人群。此外,在迁移后,检测到高度趋化和非趋化细胞,并证明可行的差异分析它们的差异。此外,我们修改了迁移通道以类似淋巴细胞,以更好地了解某些癌细胞如何通过几何限制空间移动。

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