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Engineering spheroids potentiating cell-cell and cell-ECM interactions by self-assembly of stem cell microlayer

机译:通过干细胞微层的自组装增强细胞 - 细胞和细胞-ECM相互作用的工程球体

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Numerous methods have been reported for the fabrication of 3D multi-cellular spheroids and their use in stem cell culture. Current methods typically relying on the self-assembly of trypsinized, suspended stem cells, however, show limitations with respect to cell viability, throughput, and accurate recapitulation of the natural microenvironment. In this study, we developed a new system for engineering cell spheroids by self-assembly of micro-scale monolayer of stem cells. We prepared synthetic hydrogels with the surface of chemically formed micropatterns (squares/circles with width/diameter of 200 mu m) on which mesenchymal stem cells isolated from human nasal turbinate tissue (hTMSC5) were selectively attached and formed a monolayer. The hydrogel is capable of thermally controlled expansion. As the temperature was decreased from 37 to 4 degrees C, the cell layer detached rapidly (10 min) and assembled to form spheroids with consistent size (similar to 100 mu m) and high viability (90%). Spheroidization was significantly delayed and occurred with reduced efficiency on circle patterns compared to square patterns. Multi physics mapping supported that delamination of the micro-scale monolayer may be affected by stress concentrated at the corners of the square pattern. In contrast, stress was distributed symmetrically along the boundary of the circle pattern. In addition, treatment of the micro-scale monolayer with a ROCK inhibitor significantly retarded spheroidization, highlighting the importance of contraction mediated by actin stress fibers for the stable generation of spheroidal stem cell structures. Spheroids prepared from the assembly of monolayers showed higher expression, both on the mRNA and protein levels, of ECM proteins (fibronectin and laminin) and stemness markers (Oct4, Sox2, and Nanog) compared to spheroids prepared from low-attachment plates, in which trypsinized single cells are assembled. The hTMSC spheroids also presented enhanced expression levels of markers related to tri-lineage (osteogenic, chondrogenic and adipogenic) differentiation. The changes in microcellular environments and functionalities were double-confirmed by using adipose derived mesenchymal stem cells (ADSCs). This spheroid engineering technique may have versatile applications in regenerative medicine for functionally improved 3D culture and therapeutic cell delivery. (C) 2018 Elsevier Ltd. All rights reserved.
机译:已经报道了许多方法用于制造3D多细胞球体及其在干细胞培养中的用途。然而,目前的方法通常依赖于胰蛋白酶化,悬浮的干细胞的自组装,并显示关于细胞活力,产量和自然微环境的准确综合的限制。在这项研究中,我们通过微级单层的干细胞的自组装开发了一种用于工程细胞球体的新系统。我们使用化学形成的微图(具有宽度/直径为200μm的正方形/圆形)的合成水凝胶在其上选择性地附着和形成单层,形成从人鼻鼻甲组织(HTMSC5)的间充质干细胞的表面。水凝胶能够热控制的膨胀。随着温度从37至4℃降低,电池层迅速地脱离(+ 10分钟)并组装以形成具有一致尺寸(类似于100μm)和高活力(& 90%)的球状体。与方形图案相比,球化显着延迟并发生了降低的圆形图案效率。多种物理映射支持,将微级单层的分层可能受到正方形图案的角落中浓缩的应力的影响。相反,应力沿着圆形图案的边界对称地分布。此外,用岩石抑制剂治疗微级单层显着延迟球化,突出了肌动蛋白应力纤维介导的收缩的重要性,用于稳定的球形干细胞结构。与由低附接板制备的球状体相比,由单层组装组合物制备的MRNA和蛋白质水平的表达均显示出更高的mRNA和蛋白水平,均在组装胰蛋白酶化的单细胞。 HTMSC球体还呈现了与三谱系(成骨,软骨)分化相关的增强的表达水平。通过使用脂肪衍生的间充质干细胞(ADSCs),通过使用脂肪衍生的间充质干细胞(ADSC)进行双细胞环境和功能的变化。这种球形工程技术可以在再生药物中具有多功能应用,用于功能改善的3D培养和治疗细胞输送。 (c)2018年elestvier有限公司保留所有权利。

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