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Optimizing an Osteosarcoma-Fibroblast Coculture Model to Study Antitumoral Activity of Magnesium-Based Biomaterials

机译:优化骨肉瘤 - 成纤维细胞共培养模型以研究镁基生物材料的抗肿瘤活性

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摘要

Osteosarcoma is among the most common cancers in young patients and is responsible for one-tenth of all cancer-related deaths in children. Surgery often leads to bone defects in excised tissue, while residual cancer cells may remain. Degradable magnesium alloys get increasing attention as orthopedic implants, and some studies have reported potential antitumor activity. However, most of the studies do not take the complex interaction between malignant cells and their surrounding stroma into account. Here, we applied a coculture model consisting of green fluorescent osteosarcoma cells and red fluorescent fibroblasts on extruded Mg and Mg–6Ag with a tailored degradation rate. In contrast to non-degrading Ti-based material, both Mg-based materials reduced relative tumor cell numbers. Comparing the influence of the material on a sparse and dense coculture, relative cell numbers were found to be statistically different, thus relevant, while magnesium alloy degradations were observed as cell density-independent. We concluded that the sparse coculture model is a suitable mechanistic system to further study the antitumor effects of Mg-based material.
机译:骨肉瘤是年轻患者最常见的癌症中,并负责儿童所有癌症相关死亡的十分之一。手术经常导致切除的组织中的骨缺损,而残留的癌细胞可能存在。可降解的镁合金随着矫形植入物而越来越受到关注,一些研究报告了潜在的抗肿瘤活性。然而,大多数研究并未考虑恶性细胞与其周围基质之间的复杂相互作用。在这里,我们应用了由绿色荧光骨肉瘤细胞和红色荧光成纤维细胞的共培养模型,并以挤出的Mg和Mg-6Ag,具有量身定制的降解速率。与非降解的基于Ti的材料相反,均基于Mg的材料相对肿瘤细胞数减少。比较材料对稀疏和致密共甘露水的影响,发现相对细胞数在统计学上不同,因此相关,而镁合金降解被观察为细胞密度无关。我们得出结论,稀疏的共培养模型是一种合适的机制系统,以进一步研究基于Mg的材料的抗肿瘤作用。

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