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Core-shell hydrogel beads with extracellular matrix for tumor spheroid formation

机译:具有细胞外基质的核-壳水凝胶珠粒用于形成肿瘤球体

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摘要

Creating multicellular tumor spheroids is critical for characterizing anticancer treatments since they may provide a better model of the tumor than conventional monolayer culture. Moreover, tumor cell interaction with the extracellular matrix can determine cell organization and behavior. In this work, a microfluidic system was used to form cell-laden core-shell beads which incorporate elements of the extracellular matrix and support the formation of multicellular spheroids. The bead core (comprising a mixture of alginate, collagen, and reconstituted basement membrane, with gelation by temperature control) and shell (comprising alginate hydrogel, with gelation by ionic crosslinking) were simultaneously formed through flow focusing using a cooled flow path into the microfluidic chip. During droplet gelation, the alginate acts as a fast-gelling shell which aids in preventing droplet coalescence and in maintaining spherical droplet geometry during the slower gelation of the collagen and reconstituted basement membrane components as the beads warm up. After droplet gelation, the encapsulated MCF-7 cells proliferated to form uniform spheroids when the beads contained all three components: alginate, collagen, and reconstituted basement membrane. The dose-dependent response of the MCF-7 cell tumor spheroids to two anticancer drugs, docetaxel and tamoxifen, was compared to conventional monolayer culture.
机译:创建多细胞肿瘤球体对于表征抗癌治疗至关重要,因为与常规的单层培养相比,它们可以提供更好的肿瘤模型。此外,肿瘤细胞与细胞外基质的相互作用可以决定细胞的组织和行为。在这项工作中,微流控系统被用来形成充满细胞的核-壳珠,其结合了细胞外基质的元素并支持多细胞球体的形成。通过使用冷却流路进入流动,通过流聚焦同时形成珠核(包含藻酸盐,胶原蛋白和重构的基底膜的混合物,并通过温度控制进行凝胶化)和外壳(包含藻酸盐水凝胶,通过离子交联进行凝胶化)。芯片。在液滴胶凝过程中,藻酸盐充当快速胶凝壳,有助于防止液滴聚结并在胶原蛋白和重构的基底膜成分在珠粒变热时较慢的凝胶化过程中保持液滴的球形几何形状。液滴胶凝后,当微珠包含所有三个成分:藻酸盐,胶原蛋白和重构的基底膜时,封装的MCF-7细胞增殖形成均匀的球体。将MCF-7细胞肿瘤球体对两种抗癌药物多西他赛和他莫昔芬的剂量依赖性反应与常规单层培养进行了比较。

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