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利用自组织血管化基质构建介观 3D 肿瘤模型。

Engineering Mesoscopic 3D Tumor Models with a Self-Organizing Vascularized Matrix.

机构信息

Department of Nanomedicine and Theranostics, Institute for Experimental Molecular Imaging (ExMI), RWTH Aachen University Hospital, 52074, Aachen, Germany.

Mildred Scheel School of Oncology (MSSO), Center for Integrated Oncology Aachen Bonn Cologne Düsseldorf (CIOABCD), RWTH Aachen University Hospital, 52074, Aachen, Germany.

出版信息

Adv Mater. 2024 Feb;36(5):e2303196. doi: 10.1002/adma.202303196. Epub 2023 Nov 10.

DOI:10.1002/adma.202303196
PMID:37865947
Abstract

Advanced in vitro systems such as multicellular spheroids and lab-on-a-chip devices have been developed, but often fall short in reproducing the tissue scale and self-organization of human diseases. A bioprinted artificial tumor model is introduced with endothelial and stromal cells self-organizing into perfusable and functional vascular structures. This model uses 3D hydrogel matrices to embed multicellular tumor spheroids, allowing them to grow to mesoscopic scales and to interact with endothelial cells. It is shown that angiogenic multicellular tumor spheroids promote the growth of a vascular network, which in turn further enhances the growth of cocultivated tumor spheroids. The self-developed vascular structure infiltrates the tumor spheroids, forms functional connections with the bioprinted endothelium, and can be perfused by erythrocytes and polystyrene microspheres. Moreover, cancer cells migrate spontaneously from the tumor spheroid through the self-assembled vascular network into the fluid flow. Additionally, tumor type specific characteristics of desmoplasia, angiogenesis, and metastatic propensity are preserved between patient-derived samples and tumors derived from this same material growing in the bioreactors. Overall, this modular approach opens up new avenues for studying tumor pathophysiology and cellular interactions in vitro, providing a platform for advanced drug testing while reducing the need for in vivo experimentation.

摘要

已经开发出了诸如多细胞球体和芯片上实验室等先进的体外系统,但它们往往无法重现组织规模和人类疾病的自我组织。本文引入了一种生物打印的人工肿瘤模型,其中内皮细胞和基质细胞自我组织成可灌注和功能的血管结构。该模型使用 3D 水凝胶基质来嵌入多细胞肿瘤球体,使其能够生长到介观尺度并与内皮细胞相互作用。结果表明,血管生成的多细胞肿瘤球体促进了血管网络的生长,而血管网络的生长又进一步促进了共培养肿瘤球体的生长。自组织的血管结构渗透到肿瘤球体中,与生物打印的内皮形成功能连接,并可被红细胞和聚苯乙烯微球灌注。此外,癌细胞可自发地从肿瘤球体通过自组装的血管网络迁移到流体流动中。此外,源自患者样本的肿瘤与在生物反应器中生长的相同材料衍生的肿瘤之间保留了间充质、血管生成和转移倾向的肿瘤类型特异性特征。总的来说,这种模块化方法为体外研究肿瘤病理生理学和细胞相互作用开辟了新途径,为高级药物测试提供了平台,同时减少了对体内实验的需求。

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