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利用微流控技术和图像分析对混合胶原蛋白-基质胶支架中三维癌细胞迁移进行表征

Characterization of three-dimensional cancer cell migration in mixed collagen-Matrigel scaffolds using microfluidics and image analysis.

作者信息

Anguiano María, Castilla Carlos, Maška Martin, Ederra Cristina, Peláez Rafael, Morales Xabier, Muñoz-Arrieta Gorka, Mujika Maite, Kozubek Michal, Muñoz-Barrutia Arrate, Rouzaut Ana, Arana Sergio, Garcia-Aznar José Manuel, Ortiz-de-Solorzano Carlos

机构信息

Laboratory of Preclinical Models and Analytical Tools, Division of Solid Tumors and Biomarkers, Center for Applied Medical Research and CIBERONC, Pamplona, Navarra, Spain.

Centre for Biomedical Image Analysis, Faculty of Informatics, Masaryk University, Brno, Czech Republic.

出版信息

PLoS One. 2017 Feb 6;12(2):e0171417. doi: 10.1371/journal.pone.0171417. eCollection 2017.

Abstract

Microfluidic devices are becoming mainstream tools to recapitulate in vitro the behavior of cells and tissues. In this study, we use microfluidic devices filled with hydrogels of mixed collagen-Matrigel composition to study the migration of lung cancer cells under different cancer invasion microenvironments. We present the design of the microfluidic device, characterize the hydrogels morphologically and mechanically and use quantitative image analysis to measure the migration of H1299 lung adenocarcinoma cancer cells in different experimental conditions. Our results show the plasticity of lung cancer cell migration, which turns from mesenchymal in collagen only matrices, to lobopodial in collagen-Matrigel matrices that approximate the interface between a disrupted basement membrane and the underlying connective tissue. Our quantification of migration speed confirms a biphasic role of Matrigel. At low concentration, Matrigel facilitates migration, most probably by providing a supportive and growth factor retaining environment. At high concentration, Matrigel slows down migration, possibly due excessive attachment. Finally, we show that antibody-based integrin blockade promotes a change in migration phenotype from mesenchymal or lobopodial to amoeboid and analyze the effect of this change in migration dynamics, in regards to the structure of the matrix. In summary, we describe and characterize a robust microfluidic platform and a set of software tools that can be used to study lung cancer cell migration under different microenvironments and experimental conditions. This platform could be used in future studies, thus benefitting from the advantages introduced by microfluidic devices: precise control of the environment, excellent optical properties, parallelization for high throughput studies and efficient use of therapeutic drugs.

摘要

微流控装置正成为在体外重现细胞和组织行为的主流工具。在本研究中,我们使用填充有胶原蛋白-基质胶混合成分水凝胶的微流控装置,来研究不同癌症侵袭微环境下肺癌细胞的迁移。我们展示了微流控装置的设计,从形态学和力学方面对水凝胶进行了表征,并使用定量图像分析来测量不同实验条件下H1299肺腺癌细胞的迁移。我们的结果显示了肺癌细胞迁移的可塑性,其迁移方式从仅在胶原蛋白基质中的间充质样,转变为在接近破损基底膜与下方结缔组织界面的胶原蛋白-基质胶基质中的叶足样。我们对迁移速度的量化证实了基质胶的双相作用。在低浓度时,基质胶促进迁移,很可能是通过提供一个支持性且能保留生长因子的环境。在高浓度时,基质胶减缓迁移,可能是由于过度附着。最后,我们表明基于抗体的整合素阻断促进了迁移表型从间充质样或叶足样向阿米巴样的转变,并分析了这种迁移动力学变化对基质结构的影响。总之,我们描述并表征了一个强大的微流控平台和一套软件工具,可用于研究不同微环境和实验条件下的肺癌细胞迁移。该平台可用于未来的研究,从而受益于微流控装置带来的优势:环境的精确控制、出色的光学特性、用于高通量研究的并行化以及治疗药物的高效利用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2d28/5293277/3f2dd20370d3/pone.0171417.g001.jpg

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