基于模块化组装的肝组织工程松散包装与内皮化共培养肝组织元件方法。

ty10086 提交于 周三, 08/25/2021 - 16:42
文章英文标题
Modular assembly-based approach of loosely packing co-cultured hepatic tissue elements with endothelialization for liver tissue engineering.
正文
在肝组织工程中,将肝细胞与典型的非实质性肝细胞共培养形成细胞集落,可以模拟体内微环境,促进细胞生物学功能。采用模块化组装方法,可将内皮化的肝细胞集合体进行灌注培养,从而可构建大规模的肝组织。由于紧密堆积的聚集体容易相互融合并阻碍灌注流,本研究引入了一种松散堆积模式,利用透氧聚二甲基硅氧烷( PDMS )基微阱装置,通过共培养肝癌( HepG2 )细胞、瑞士3T3细胞和人脐静脉内皮细胞( HUVECs ),获得高密度的内皮细胞聚集体作为肝组织元素,然后将共培养的聚集体在PDMS生物反应器中进行灌注培养10 d。为了维持合适的间质空间以稳定灌注,采用可降解聚乳酸( PLLA )支架纤维与聚集体混合,形成松散的填充模式。在微井共培养中,瑞士3T3细胞对肝细胞聚集体的形成有显著的贡献。HUVECs在聚集物中形成外周分布,供内皮化。在灌流培养中,与纯HepG2聚集体相比,HepG2 / Swiss 3T3 / HUVECs共培养聚集体表现出更高的细胞增殖和肝脏特异性功能表达(即葡萄糖消耗和白蛋白分泌)。在松装模式下,共培养聚集体表现出细胞迁移和与纤维粘连的特征性组织学形态。将HepG2、Swiss 3T3和HUVECs共培养,观察到Swiss 3T3细胞有利于内皮细胞聚集的形成。松散的聚集体使长期灌注培养具有高活性和生物学功能。本研究将指导我们采用基于骨料的模块化组装方式构建大规模肝组织模型。
文章内容(英文)
In liver tissue engineering, co-culturing hepatocytes with typical non-parenchymal hepatic cells to form cell aggregates is available to mimic the in vivo microenvironment and promote cell biological functions. With a modular assembly approach, endothelialized hepatic cell aggregates can be packed for perfusion culture, which enables the construction of large-scale liver tissues. Since tightly packed aggregates tend to fuse with each other and block perfusion flows, a loosely packed mode was introduced in our study.;Using an oxygen-permeable polydimethylsiloxane (PDMS)-based microwell device, highly dense endothelialized hepatic cell aggregates were generated as hepatic tissue elements by co-culturing hepatocellular carcinoma (HepG2) cells, Swiss 3T3 cells, and human umbilical vein endothelial cells (HUVECs). The co-cultured aggregates were then harvested and applied in a PDMS-fabricated bioreactor for 10 days of perfusion culture. To maintain appropriate interstitial spaces for stable perfusion, biodegradable poly-L-lactic acid (PLLA) scaffold fibers were used and mixed with the aggregates, forming a loosely packed mode.;In a microwell co-culture, Swiss 3T3 cells significantly contributed to the formation of hepatic cell aggregates. HUVECs developed a peripheral distribution in aggregates for endothelialization. In the perfusion culture, compared with pure HepG2 aggregates, HepG2/Swiss 3T3/HUVECs co-cultured aggregates exhibited a higher level of cell proliferation and liver-specific function expression (i.e., glucose consumption and albumin secretion). Under the loosely packed mode, co-cultured aggregates showed a characteristic histological morphology with cell migration and adhesion to fibers. The assembled hepatic tissue elements were obtained with 32% of in vivo cell density.;In a co-culture of HepG2, Swiss 3T3, and HUVECs, Swiss 3T3 cells were observed to be beneficial for the formation of endothelialized hepatic cell aggregates. Loosely packed aggregates enabled long-term perfusion culture with high viability and biological function. This study will guide us in constructing large-scale liver tissue models by way of aggregate-based modular assembly.
来源出处
Journal|[J]Annals of Translational MedicineVolume 8, Issue 21. 2020. PP 1400-1400
DOI
https://doi.org/10.21037/ATM-20-1598

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