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A spheroid toxicity assay using magnetic 3D bioprinting and real-time mobile device-based imaging

机译:使用磁性3D生物打印和基于实时移动设备的成像的球体毒性测定

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An ongoing challenge in biomedical research is the search for simple, yet robust assays using 3D cell cultures for toxicity screening. This study addresses that challenge with a novel spheroid assay, wherein spheroids, formed by magnetic 3D bioprinting, contract immediately as cells rearrange and compact the spheroid in relation to viability and cytoskeletal organization. Thus, spheroid size can be used as a simple metric for toxicity. The goal of this study was to validate spheroid contraction as a cytotoxic endpoint using 3T3 fibroblasts in response to 5 toxic compounds (all-trans retinoic acid, dexamethasone, doxorubicin, 5′-fluorouracil, forskolin), sodium dodecyl sulfate (+control), and penicillin-G (?control). Real-time imaging was performed with a mobile device to increase throughput and efficiency. All compounds but penicillin-G significantly slowed contraction in a dose-dependent manner (Z’?=?0.88). Cells in 3D were more resistant to toxicity than cells in 2D, whose toxicity was measured by the MTT assay. Fluorescent staining and gene expression profiling of spheroids confirmed these findings. The results of this study validate spheroid contraction within this assay as an easy, biologically relevant endpoint for high-throughput compound screening in representative 3D environments.
机译:生物医学研究中的一项持续挑战是寻找使用3D细胞培养物进行毒性筛选的简单而稳健的测定方法。这项研究通过一种新颖的球状体分析方法解决了这一挑战,其中通过磁性3D生物打印形成的球状体会随着细胞重新排列并压缩与生命力和细胞骨架组织有关的球状体而立即收缩。因此,球体尺寸可以用作毒性的简单度量。这项研究的目的是使用3T3成纤维细胞对5种有毒化合物(全反式维甲酸,地塞米松,阿霉素,5'-氟尿嘧啶,福司可林),十二烷基硫酸钠(+对照),和青霉素-G(对照)。使用移动设备执行实时成像以提高吞吐量和效率。除青霉素-G外,所有化合物均以剂量依赖性方式显着减慢了收缩(Z’≤0.88)。 3D细胞比2D细胞具有更高的抗毒性,而2D细胞的毒性是通过MTT分析测定的。球体的荧光染色和基因表达谱证实了这些发现。这项研究的结果验证了此测定法中的球状体收缩是在代表性3D环境中进行高通量化合物筛选的简单,生物学相关的终点。

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