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细胞胶囊作为一种工具,用于生产多细胞球体,并用于研究体外肿瘤进展的力学。

Cellular capsules as a tool for multicellular spheroid production and for investigating the mechanics of tumor progression in vitro.

机构信息

Institut Curie, 75005 Paris, France.

出版信息

Proc Natl Acad Sci U S A. 2013 Sep 10;110(37):14843-8. doi: 10.1073/pnas.1309482110. Epub 2013 Aug 26.

Abstract

Deciphering the multifactorial determinants of tumor progression requires standardized high-throughput preparation of 3D in vitro cellular assays. We present a simple microfluidic method based on the encapsulation and growth of cells inside permeable, elastic, hollow microspheres. We show that this approach enables mass production of size-controlled multicellular spheroids. Due to their geometry and elasticity, these microcapsules can uniquely serve as quantitative mechanical sensors to measure the pressure exerted by the expanding spheroid. By monitoring the growth of individual encapsulated spheroids after confluence, we dissect the dynamics of pressure buildup toward a steady-state value, consistent with the concept of homeostatic pressure. In turn, these confining conditions are observed to increase the cellular density and affect the cellular organization of the spheroid. Postconfluent spheroids exhibit a necrotic core cemented by a blend of extracellular material and surrounded by a rim of proliferating hypermotile cells. By performing invasion assays in a collagen matrix, we report that peripheral cells readily escape preconfined spheroids and cell-cell cohesivity is maintained for freely growing spheroids, suggesting that mechanical cues from the surrounding microenvironment may trigger cell invasion from a growing tumor. Overall, our technology offers a unique avenue to produce in vitro cell-based assays useful for developing new anticancer therapies and to investigate the interplay between mechanics and growth in tumor evolution.

摘要

要破译肿瘤进展的多因素决定因素,需要标准化的高通量制备 3D 体外细胞分析。我们提出了一种基于细胞包封和在可渗透、弹性、中空微球内生长的简单微流控方法。我们表明,这种方法能够大规模生产尺寸可控的多细胞球体。由于其几何形状和弹性,这些微胶囊可以作为独特的定量机械传感器,用于测量由扩展球体施加的压力。通过监测融合后单个封装球体的生长,我们剖析了朝向稳定状态值的压力建立动力学,这与稳态压力的概念一致。反过来,这些约束条件被观察到会增加细胞密度并影响球体的细胞组织。融合后的球体表现出由细胞外基质混合物固定的坏死核心,并被增殖的超运动细胞的边缘包围。通过在胶原基质中进行侵袭实验,我们报告说,周围细胞很容易从预先限制的球体中逃逸,并且对于自由生长的球体,细胞间黏附性得以维持,这表明来自周围微环境的机械线索可能会触发肿瘤生长时的细胞侵袭。总体而言,我们的技术为体外基于细胞的测定提供了独特的途径,这些测定可用于开发新的抗癌疗法,并研究机械和生长在肿瘤进化中的相互作用。

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