Brain Cancer Cell-Derived Matrices and Effects on Astrocyte Migration.

IF 2.9 4区 生物学 Q1 ANATOMY & MORPHOLOGY Cells Tissues Organs Pub Date : 2023-01-01 Epub Date: 2022-02-15 DOI:10.1159/000522609
Rebecca Louisthelmy, Brycen M Burke, R Chase Cornelison
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引用次数: 1

Abstract

Cell-derived matrices are useful tools for studying the extracellular matrix (ECM) of different cell types and testing the effects on cell migration or wound repair. These matrices typically are generated using extended culture with ascorbic acid to boost ECM production. Applying this technique to cancer cell cultures could advance the study of cancer ECM and its effects on recruitment and training of the tumor microenvironment, but ascorbic acid is potently cytotoxic to cancer cells. Macromolecular crowding (MMC) agents can also be added to increase matrix deposition based on the excluded volume principle. We report the use of MMC alone as an effective strategy to generate brain cancer cell-derived matrices for downstream analyses and cell migration studies. We cultured the mouse glioblastoma cell line GL261 for 1 week in the presence of three previously reported MMC agents (carrageenan, Ficoll 70/400, and hyaluronic acid). We measured the resulting deposition of collagens and sulfated glycosaminoglycans using quantitative assays, as well as other matrix components by immunostaining. Both carrageenan and Ficoll promoted significantly more accumulation of total collagen content, sulfated glycosaminoglycan content, and fibronectin staining. Only Ficoll, however, also demonstrated a significant increase in collagen I staining. The results were more variable in 3D spheroid culture. We focused on Ficoll MMC matrices, which were isolated using the small molecule Raptinal to induce cancer cell apoptosis and matrix decellularization. The cancer cell-derived matrix promoted significantly faster migration of human astrocytes in a scratch wound assay, which may be explained by focal adhesion morphology and an increase in cellular metabolic activity. Ultimately, these data show MMC culture is a useful technique to generate cancer cell-derived matrices and study the effects on stromal cell migration related to wound repair.

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脑癌细胞衍生基质及其对星形胶质细胞迁移的影响
细胞衍生基质是研究不同类型细胞的细胞外基质(ECM)以及测试其对细胞迁移或伤口修复的影响的有用工具。这些基质通常是用抗坏血酸延长培养产生的,以促进 ECM 的生成。将这种技术应用于癌细胞培养可推进对癌症 ECM 及其对肿瘤微环境招募和训练的影响的研究,但抗坏血酸对癌细胞有强烈的细胞毒性。根据排除体积原理,还可以添加大分子拥挤剂(MMC)来增加基质沉积。我们报告了单独使用 MMC 作为生成脑癌细胞衍生基质的有效策略,用于下游分析和细胞迁移研究。我们将小鼠胶质母细胞瘤细胞系 GL261 在之前报道过的三种 MMC 制剂(卡拉胶、Ficoll 70/400 和透明质酸)存在下培养 1 周。我们使用定量测定法测量了胶原和硫酸化糖胺聚糖的沉积情况,并通过免疫染色法测量了其他基质成分的沉积情况。角叉菜胶和 Ficoll 都能促进总胶原含量、硫酸化氨基糖含量和纤连蛋白染色的明显增加。不过,只有 Ficoll 也显示出胶原蛋白 I 染色的显著增加。三维球形培养的结果变化较大。我们重点研究了Ficoll MMC基质,它是利用小分子Raptinal诱导癌细胞凋亡和基质脱细胞而分离出来的。在划痕伤口试验中,癌细胞衍生基质明显加快了人类星形胶质细胞的迁移速度,这可能与病灶粘附形态和细胞代谢活动增加有关。这些数据最终表明,MMC 培养是生成癌细胞衍生基质和研究与伤口修复相关的基质细胞迁移效应的有用技术。
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来源期刊
Cells Tissues Organs
Cells Tissues Organs 生物-发育生物学
CiteScore
4.90
自引率
3.70%
发文量
45
审稿时长
6-12 weeks
期刊介绍: ''Cells Tissues Organs'' aims at bridging the gap between cell biology and developmental biology and the emerging fields of regenerative medicine (stem cell biology, tissue engineering, artificial organs, in vitro systems and transplantation biology). CTO offers a rapid and fair peer-review and exquisite reproduction quality. Special topic issues, entire issues of the journal devoted to a single research topic within the range of interests of the journal, are published at irregular intervals.
期刊最新文献
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