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A 3D Bioprinted Material That Recapitulates the Perivascular Bone Marrow Structure for Sustained Hematopoietic and Cancer Models

机译:用于持续造血和癌症模型的血管骨髓结构的3D生物印刷材料

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摘要

Translational medicine requires facile experimental systems to replicate the dynamic biological systems of diseases. Drug approval continues to lag, partly due to incongruencies in the research pipeline that traditionally involve 2D models, which could be improved with 3D models. The bone marrow (BM) poses challenges to harvest as an intact organ, making it difficult to study disease processes such as breast cancer (BC) survival in BM, and to effective evaluation of drug response in BM. Furthermore, it is a challenge to develop 3D BM structures due to its weak physical properties, and complex hierarchical structure and cellular landscape. To address this, we leveraged 3D bioprinting to create a BM structure with varied methylcellulose (M): alginate (A) ratios. We selected hydrogels containing 4% (w/v) M and 2% (w/v) A, which recapitulates rheological and ultrastructural features of the BM while maintaining stability in culture. This hydrogel sustained the culture of two key primary BM microenvironmental cells found at the perivascular region, mesenchymal stem cells and endothelial cells. More importantly, the scaffold showed evidence of cell autonomous dedifferentiation of BC cells to cancer stem cell properties. This scaffold could be the platform to create BM models for various diseases and also for drug screening.
机译:翻译药物需要易于实验系统来复制动态生物系统的疾病。药物批准继续滞后,部分原因是传统上涉及2D型号的研究管道的不协调,这可以通过3D模型来改进。骨髓(BM)造成挑战以作为完整器官收获,使得难以研究BM中乳腺癌(BC)存活的疾病过程,并有效评估BM中的药物反应。此外,由于其弱的物理性质,以及复杂的层次结构和蜂窝景观,它是一种挑战。为了解决这一点,我们利用3D BioPlinting以不同的甲基纤维素(m)产生BM结构:藻酸盐(a)比率。我们选择含有4%(w / v)m和2%(w / v)a的水凝胶,其概述了Bm的流变和超微结构特征,同时保持培养稳定性。该水凝胶持续了在细节血管区,间充质干细胞和内皮细胞处发现的两个关键原发性BM微环境细胞的培养。更重要的是,支架显示出对癌症干细胞性能的BC细胞的细胞自主分泌剂的证据。这种脚手架可以是为各种疾病创建BM模型的平台,也可以用于药物筛查。

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