Gelatin methacryloyl and Laponite bioink for 3D bioprinted organotypic tumor modeling

自愈水凝胶 明胶 细胞外基质 材料科学 生物加工 旁分泌信号 组织工程 生物医学工程 纳米技术 复合数 三维细胞培养 生物物理学 细胞 化学 高分子化学 复合材料 生物化学 生物 医学 受体
作者
Natan Roberto de Barros,Alejandro Palomar Gómez,Menekşe Ermis,Natashya Falcone,Reihaneh Haghniaz,Patric Young,Yaqi Gao,Albert-Fred Aquino,Siyuan Li,Siyi Niu,RunRun Chen,Shuyi Huang,Yangzhi Zhu,Payam Eliahoo,Arthur Sun,Danial Khorsandi,Jinjoo Kim,Jonathan A. Kelber,Ali Khademhosseini,Han‐Jun Kim
出处
期刊:Biofabrication [IOP Publishing]
卷期号:15 (4): 045005-045005 被引量:15
标识
DOI:10.1088/1758-5090/ace0db
摘要

Abstract Three-dimensional (3D) in vitro tumor models that can capture the pathophysiology of human tumors are essential for cancer biology and drug development. However, simulating the tumor microenvironment is still challenging because it consists of a heterogeneous mixture of various cellular components and biological factors. In this regard, current extracellular matrix (ECM)-mimicking hydrogels used in tumor tissue engineering lack physical interactions that can keep biological factors released by encapsulated cells within the hydrogel and improve paracrine interactions. Here, we developed a nanoengineered ion-covalent cross-linkable bioink to construct 3D bioprinted organotypic tumor models. The bioink was designed to implement the tumor ECM by creating an interpenetrating network composed of gelatin methacryloyl (GelMA), a light cross-linkable polymer, and synthetic nanosilicate (Laponite) that exhibits a unique ionic charge to improve retention of biological factors released by the encapsulated cells and assist in paracrine signals. The physical properties related to printability were evaluated to analyze the effect of Laponite hydrogel on bioink. Low GelMA (5%) with high Laponite (2.5%–3.5%) composite hydrogels and high GelMA (10%) with low Laponite (1.0%–2.0%) composite hydrogels showed acceptable mechanical properties for 3D printing. However, a low GelMA composite hydrogel with a high Laponite content could not provide acceptable cell viability. Fluorescent cell labeling studies showed that as the proportion of Laponite increased, the cells became more aggregated to form larger 3D tumor structures. Reverse transcription-polymerase chain reaction (RT-qPCR) and western blot experiments showed that an increase in the Laponite ratio induces upregulation of growth factor and tissue remodeling-related genes and proteins in tumor cells. In contrast, cell cycle and proliferation-related genes were downregulated. On the other hand, concerning fibroblasts, the increase in the Laponite ratio indicated an overall upregulation of the mesenchymal phenotype-related genes and proteins. Our study may provide a rationale for using Laponite-based hydrogels in 3D cancer modeling.
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