论文标题

共培养球体的结构调节3D细胞外基质内的肿瘤入侵

The architecture of co-culture spheroids regulates tumor invasion within a 3D extracellular matrix

论文作者

Huang, Yu Ling, Shiau, Carina, Wu, Cindy, Segall, Jeffrey E., Wu, Mingming

论文摘要

肿瘤侵袭是肿瘤细胞脱离原发性肿瘤并进入血管系统的过程,是癌症转移的重要一步。当前的大多数3D肿瘤入侵测定法由嵌入细胞外基质(ECM)中的单个肿瘤细胞组成。这些测定法教会了我们今天对关键生物物理(例如ECM刚度)和生化(例如细胞因子梯度)参数中如何在肿瘤微环境中引导和调节肿瘤浸润的内容。单个肿瘤细胞浸润测定法的一个局限性是,它没有考虑肿瘤内细胞 - 细胞粘附。在本文中,我们开发了与微观成像兼容的千分尺3D共培养球体入侵测定。千分尺尺度共培养球体(转移性乳腺癌MDA-MB-231的1:1比率和非肿瘤上皮MCF-10A细胞)使用一系列微孔制成,然后将其嵌入胶原蛋白基质中。肿瘤球体侵袭的实时成像表明,肿瘤球体内两种细胞类型的空间分布受到严格调节的肿瘤侵袭。这项工作将肿瘤结构与肿瘤侵袭联系起来,并强调了肿瘤大部分肿瘤侵袭中生物物理提示的重要性。

Tumor invasion, the process by which tumor cells break away from their primary tumor and gain access to vascular systems, is an important step in cancer metastasis. Most current 3D tumor invasion assays consisted of single tumor cells embedded within an extracellular matrix (ECM). These assays taught us much of what we know today on how key biophysical (e.g. ECM stiffness) and biochemical (e.g. cytokine gradients) parameters within the tumor microenvironment guided and regulated tumor invasion. One limitation of the single tumor cell invasion assay was that it did not account for cell-cell adhesion within the tumor. In this article, we developed a micrometer scale 3D co-culture spheroid invasion assay that was compatible with microscopic imaging. Micrometer scale co-culture spheroids (1:1 ratio of metastatic breast cancer MDA-MB-231 and non-tumorigenic epithelial MCF-10A cells) were made using an array of microwells, and then were embedded within a collagen matrix in a microfluidic platform. Real time imaging of tumor spheroid invasion revealed that the spatial distribution of the two cell types within the tumor spheroid critically regulated tumor invasion. This work linked tumor architecture with tumor invasion and highlighted the importance of the biophysical cues within the bulk of the tumor in tumor invasion.

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